Treatment of Patients With Major Depressive Disorder PRACTICE GUIDELINE FOR THE

Transcription

Treatment of Patients With Major Depressive Disorder PRACTICE GUIDELINE FOR THE
PRACTICE GUIDELINE FOR THE
Treatment of Patients With
Major Depressive Disorder
Third Edition
WORK GROUP ON MAJOR DEPRESSIVE DISORDER
Alan J. Gelenberg, M.D., Chair
Marlene P. Freeman, M.D.
John C. Markowitz, M.D.
Jerrold F. Rosenbaum, M.D.
Michael E. Thase, M.D.
Madhukar H. Trivedi, M.D.
Richard S. Van Rhoads, M.D., Consultant
INDEPENDENT REVIEW PANEL
Victor I. Reus, M.D., Chair
J. Raymond DePaulo, Jr., M.D.
Jan A. Fawcett, M.D.
Christopher D. Schneck, M.D.
David A. Silbersweig, M.D.
This practice guideline was approved in May 2010 and published in October 2010. A guideline watch, summarizing
significant developments in the scientific literature since publication of this guideline, may be available at
http://www.psychiatryonline.com/pracGuide/pracGuideTopic_7.aspx.
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
FINANCIAL DISCLOSURES/CONFLICTS OF INTEREST
The Work Group on Major Depressive Disorder reports
the following potentially competing interests for the period from May 2005 to May 2010:
Dr. Gelenberg reports consulting for Eli Lilly and Company, Pfizer, Best Practice, AstraZeneca, Wyeth, Cyberonics, Novartis, Forest Pharmaceuticals, Inc., GlaxoSmithKline, ZARS Pharma, Jazz Pharmaceuticals, Lundbeck,
Takeda Pharmaceuticals North America, Inc., eResearch
Technology, Dey Pharma, PGxHealth, and Myriad Genetics. He reports serving on speakers bureaus for Pfizer,
GlaxoSmithKline, and Wyeth. He reports receiving research grant funding from Eli Lilly and Company, Pfizer,
and GlaxoSmithKline. He reports stock ownership in
Healthcare Technology Systems.
Dr. Freeman reports that she received research support
from the Meadows Foundation, the National Institute for
Mental Health, the U.S. Food and Drug Administration,
the Institute for Mental Health Research, Forest, GlaxoSmithKline and Eli Lilly and Company (investigatorinitiated trials), and Pronova Biocare (research materials).
She received an honorarium for case-based peer-reviewed
material for AstraZeneca’s website. She reports consulting
for Ther-Rx, Reliant, and Pamlab. She reports receiving
an honorarium for speaking at an APA continuing medical
education program that was sponsored by Forest and an
honorarium for speaking at a continuing medication education program sponsored by KV Pharmaceuticals. She
reports receiving an honorarium from Leerink Swann for
participating in a focus group.
Dr. Markowitz reports consulting for Ono Pharmaceutical Co., Ltd. (2005). He reports receiving research
support from Forest Pharmaceuticals, Inc. (2005). He reports receiving grant support from the National Institute
of Mental Health (2005–2013), the National Alliance for
Research in Schizophrenia and Depression (2005), and
MINT: Mental Health Initiative (2005). He reports receiving royalties from American Psychiatric Publishing, Inc.
(2005–2010), Basic Books (2005–2010), Elsevier (2005–
2010), and Oxford University Press (2007–2010).
Dr. Rosenbaum reports attending advisory boards for
Bristol-Myers Squibb, Cephalon, Cyberonics, Forest Pharmaceuticals, Inc., Eli Lilly and Company, MedAvante,
Neuronetics, Inc., Novartis, Orexigen Therapeutics, Inc.,
Organon BioSciences, Pfizer, Roche Diagnostics, Sanofiaventis, Shire, and Wyeth. He reports consulting for Auspex Pharmaceuticals, Compellis Pharmaceuticals, EPIX
Pharmaceuticals, Neuronetics, Inc., Organon BioSciences, Somaxon, and Supernus Pharmaceuticals, Inc. He
reports receiving honoraria from lectureships for Boehringer Ingleheim, Bristol-Myers Squibb, Cyberonics,
Forest Pharmaceuticals, Inc., Eli Lilly and Company, and
Schwartz Pharma. He was involved in the creation of
the Massachusetts General Hospital Psychiatry Academy
(MGH-PA) and has served as a panelist in four satellite
broadcast programs. MGH-PA programs that have industry support are always multi-sponsored, and curriculum
development by the Academy is independent of sponsorship; the curricula from January 2005 to March 2009 included sponsorship support from AstraZeneca, BristolMyers Squibb, Cephalon, Eli Lilly and Company, Forest
Pharmaceuticals, Inc., GlaxoSmithKline, Janssen Medical
Affairs LLC, Ortho-McNeil Pharmaceutical, sanofiaventis, Shire, and Wyeth. He reports equity holdings in
Compellis Pharmaceuticals, MedAvante, and Somaxon.
Dr. Thase reports that he provided scientific consultation to AstraZeneca, Bristol-Myers Squibb, Eli Lilly &
Company, Forest Pharmaceuticals, Inc., Gerson Lehman
Group, GlaxoSmithKline, Guidepoint Global, H. Lundbeck A/S, MedAvante, Inc., Neuronetics, Inc., Novartis,
Otsuka, Ortho-McNeil Pharmaceuticals, PamLab, L.L.C.,
Pfizer (formerly Wyeth-Ayerst Laboratories), ScheringPlough (formerly Organon), Shire U.S., Inc., Supernus
Pharmaceuticals, Takeda (Lundbeck), and Transcept Pharmaceuticals. He was a member of the speakers bureaus for
AstraZeneca, Bristol-Myers Squibb, Eli Lilly and Company, GlaxoSmithKline, Pfizer (formerly Wyeth-Ayerst
Laboratories), and Schering-Plough (formerly Organon).
He received grant funding from Eli Lilly and Company,
GlaxoSmithKline, the National Institute of Mental Health,
the Agency for Healthcare Research and Quality, and
Sepracor, Inc. He had equity holdings in MedAvante, Inc.,
and received royalty income from American Psychiatric
Publishing, Inc., Guilford Publications, Herald House,
Oxford University Press, and W.W. Norton and Company.
His wife was employed as the group scientific director for
Embryon (formerly Advogent), which does business with
Bristol-Myers Squibb and Pfizer/Wyeth.
Dr. Trivedi reports that he was a consultant to or on
speaker bureaus for Abbott Laboratories, Inc., Abdi Ibrahim, Akzo (Organon Pharmaceuticals, Inc.), AstraZeneca,
Bristol-Myers Squibb Company, Cephalon, Inc., Cyberonics, Inc., Eli Lilly and Company, Evotec, Fabre Kramer
Pharmaceuticals, Inc., Forest Pharmaceuticals, GlaxoSmithKline, Janssen Pharmaceutica Products, L.P., Johnson
& Johnson P.R.D., Meade-Johnson, Medtronic, Neuronetics, Otsuka Pharmaceuticals, Parke-Davis Pharmaceuti-
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
cals, Inc., Pfizer, Inc., Sepracor, Shire Development, Solvay
Pharmaceuticals, VantagePoint, and Wyeth-Ayerst Laboratories. He received research support from the Agency for
Healthcare Research and Quality, Corcept Therapeutics,
Inc., Cyberonics, Inc., Merck, National Alliance for Research in Schizophrenia and Depression, National Institute of Mental Health, National Institute on Drug Abuse,
Novartis, Pharmacia & Upjohn, Predix Pharmaceuticals
(Epix), Solvay Pharmaceuticals, Inc., and Targacept.
Dr. Van Rhoads reports no competing interests.
The Independent Review Panel, including Drs. Reus,
DePaulo, Fawcett, Schneck, and Silbersweig, report no
competing interests. The Independent Review Panel reviewed this guideline to assess potential biases and found
no evidence of influence from the industry and other relationships of the Work Group disclosed above. The
Steering Committee on Practice Guidelines also reviewed
this guideline and found no evidence of influence from
these relationships. The development process for this
guideline, including the roles of the Work Group, Independent Review Panel, Steering Committee, APA Assembly, and APA Board of Trustees is described in “Overview
of Guideline Development Process” on p. 11.
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
AMERICAN PSYCHIATRIC ASSOCIATION
STEERING COMMITTEE ON PRACTICE GUIDELINES
John S. McIntyre, M.D., Chair (1999–2009), Consultant (2009–2010)
Joel Yager, M.D., Vice-Chair (2008–2009), Chair (2009–2010)
Daniel J. Anzia, M.D.
Thomas J. Craig, M.D., M.P.H.
Molly T. Finnerty, M.D.
Bradley R. Johnson, M.D.
Francis G. Lu, M.D.
James E. Nininger, M.D., Vice-Chair (2009–2010)
Barbara Schneidman, M.D.
Paul Summergrad, M.D.
Sherwyn M. Woods, M.D., Ph.D.
Michael J. Vergare, M.D.
M. Justin Coffey, M.D. (fellow)
Kristen Ochoa, M.D. (fellow)
Jeremy Wilkinson, M.D. (fellow)
Sheila Hafter Gray, M.D. (liaison)
STAFF
Robert Kunkle, M.A., Director, Practice Guidelines Project
Robert M. Plovnick, M.D., M.S., Director, Dept. of Quality Improvement and Psychiatric Services
Darrel A. Regier, M.D., M.P.H., Director, Division of Research
MEDICAL EDITOR
Laura J. Fochtmann, M.D.
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
CONTENTS
STATEMENT OF INTENT . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 11
OVERVIEW OF GUIDELINE DEVELOPMENT PROCESS. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 11
GUIDE TO USING THIS PRACTICE GUIDELINE . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 13
OFF-LABEL USE OF MEDICATIONS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 13
INTRODUCTION . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 13
PART A: TREATMENT RECOMMENDATIONS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
I. EXECUTIVE SUMMARY . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
A. Coding System . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
B. Summary of Recommendations . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
1. Psychiatric management . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
a. Establish and maintain a therapeutic alliance . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
b. Complete the psychiatric assessment . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
c. Evaluate the safety of the patient . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
d. Establish the appropriate setting for treatment . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 16
e. Evaluate functional impairment and quality of life . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 16
f. Coordinate the patient’s care with other clinicians . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 16
g. Monitor the patient’s psychiatric status . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 16
h. Integrate measurements into psychiatric management . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 16
i. Enhance treatment adherence . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 16
j. Provide education to the patient and the family . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 16
2. Acute phase . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 17
a. Choice of an initial treatment modality . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 17
1. Pharmacotherapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 17
2. Other somatic therapies . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 17
3. Psychotherapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 17
4. Psychotherapy plus antidepressant medication . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 18
b. Assessing the adequacy of treatment response . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 18
c. Strategies to address nonresponse . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 18
3. Continuation phase . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 19
4. Maintenance phase . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 19
5. Discontinuation of treatment . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 20
6. Clinical factors influencing treatment . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 20
a. Psychiatric factors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 20
b. Demographic and psychosocial factors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 20
c. Co-occurring general medical conditions . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 21
II. FORMULATION AND IMPLEMENTATION OF A TREATMENT PLAN . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 22
A. Psychiatric Management . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 22
1. Establish and maintain a therapeutic alliance . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 23
2. Complete the psychiatric assessment. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 23
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
3. Evaluate the safety of the patient . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 25
4. Establish the appropriate setting for treatment . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 26
5. Evaluate functional impairment and quality of life . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 26
6. Coordinate the patient’s care with other clinicians . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 27
7. Monitor the patient’s psychiatric status . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 27
8. Integrate measurements into psychiatric management . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 28
9. Enhance treatment adherence . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 28
10. Provide education to the patient and the family . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 29
B. Acute Phase . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .30
1. Choice of initial treatment modality . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 30
2. Pharmacotherapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 31
a. Efficacy of antidepressant medications . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 33
1. Selective serotonin reuptake inhibitors. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 33
2. Serotonin norepinephrine reuptake inhibitors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 33
3. Other antidepressant medications . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 35
4. Tricyclic antidepressants . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 35
5. Monoamine oxidase inhibitors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 35
b. Side effects of antidepressant medications. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 36
1. Selective serotonin reuptake inhibitors. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 36
a. Gastrointestinal . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 36
b. Activation/insomnia . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 36
c. Sexual side effects . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 36
d. Neurological effects . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 38
e. Falls . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 38
f. Effects on weight . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 39
g. Serotonin syndrome . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 39
h. Drug interactions . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 39
i. Discontinuation syndrome . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 39
2. Serotonin norepinephrine reuptake inhibitors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
3. Other antidepressant medications . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
a. Bupropion . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
b. Mirtazapine . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
c. Trazodone . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
d. Nefazodone . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
4. Tricyclic antidepressants . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 41
a. Cardiovascular effects . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 41
b. Anticholinergic side effects . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 41
c. Sedation . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 41
d. Weight gain . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 41
e. Neurological effects. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 41
f. Falls . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 42
g. Medication interactions . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 42
5. Monoamine oxidase inhibitors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 42
a. Hypertensive crises . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 42
b. Serotonin syndrome . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 43
c. Cardiovascular effects . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 43
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
d. Weight gain . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 43
e. Sexual side effects . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 43
f. Neurological effects . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 43
c. Implementation of pharmacotherapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 43
3. Other somatic therapies . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 44
a. Electroconvulsive therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 44
1. Side effects of electroconvulsive therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 45
2. Implementation of electroconvulsive therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 45
b. Transcranial magnetic stimulation . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 46
c. Vagus nerve stimulation . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 46
4. Psychotherapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 46
a. Specific psychotherapies . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 47
1. Cognitive and behavioral therapies . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 47
2. Interpersonal psychotherapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 47
3. Psychodynamic psychotherapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 48
4. Problem-solving therapy. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 48
5. Marital therapy and family therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 48
6. Group therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 48
b. Implementation . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 49
c. Combining psychotherapy and medication . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 49
5. Complementary and alternative treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 50
a. St. John’s wort . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 50
b. S-adenosyl methionine . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 50
c. Omega-3 fatty acids . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 51
d. Folate . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 51
e. Light therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 51
f. Acupuncture . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 51
6. Assessing response and adequacy of treatment. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 52
7. Strategies to address incomplete response . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 52
a. Maximizing initial treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 53
b. Changing to other treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 54
c. Augmenting and combining treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 54
C. Continuation Phase . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 56
D. Maintenance Phase . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 57
E. Discontinuation of Treatment . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 58
III. SPECIFIC CLINICAL FEATURES INFLUENCING THE TREATMENT PLAN . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 59
A. Psychiatric Factors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 59
1. Depressive symptoms . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 59
a. Suicidal ideation and behaviors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 59
b Major depressive disorder–related cognitive dysfunction . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 60
2. DSM depressive subtypes . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 61
a. Psychotic features . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 61
b. Catatonic features . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 61
c. Melancholic features . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 61
d. Atypical features . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 62
e. Seasonal pattern . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 62
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
3. Co-occurring psychiatric disorders . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 62
a. Dysthymic disorder . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 62
b. Anxiety disorders . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 63
c. Dementia . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 63
d. Substance use disorders . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 63
e. Personality disorders . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 64
f. Eating disorders . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 65
B. Demographic and Psychosocial Variables . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .65
1. Major psychosocial stressors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 65
2. Bereavement . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 65
3. Culture and ethnicity . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 66
4. Older age. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 66
5. Gender . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 68
6. Pregnancy and postpartum . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 69
a. Depression during pregnancy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 69
1. Risks of antidepressants during pregnancy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 69
2. Implementation of pharmacotherapy during pregnancy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 70
b. Postpartum depression . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 71
7. Family history. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 72
C. Treatment Implications of Co-occurring General Medical Conditions . . . . . . . . . . . . . . . . . . . . . . . . . . . . .72
1. Hypertension . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 72
2. Cardiac disease . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 72
3. Stroke . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 73
4. Parkinson’s disease . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 73
5. Epilepsy. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 74
6. Obesity . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 74
7. Diabetes . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 75
8. Sleep apnea . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 75
9. Human immunodeficiency virus and hepatitis C infections . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 75
10. Pain syndromes . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 76
11. Obstructive uropathy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 77
12. Glaucoma . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 77
PART B: BACKGROUND INFORMATION AND REVIEW OF AVAILABLE EVIDENCE . . . . . . . . . . . . . . . 77
IV. DISEASE DEFINITION, EPIDEMIOLOGY, NATURAL HISTORY, AND COURSE . . . . . . . . . . . . . . . . . . . . . . . . . . . . .77
A. Disease Definition . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .77
B. Epidemiology . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .78
C. Natural History and Course . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .81
1. Recurrence . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 81
2. Interepisode status . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 81
3. Complications and prognosis . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 81
V. REVIEW AND SYNTHESIS OF AVAILABLE EVIDENCE . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .81
A. Acute Phase Somatic Treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .83
1. Antidepressant medications. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 83
a. Selective serotonin reuptake inhibitors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 83
b. Serotonin norepinephrine reuptake inhibitors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 84
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
B.
C.
D.
E.
F.
c. Other antidepressant medications . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 85
1. Bupropion . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 85
2. Mirtazapine . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 85
3. Nefazodone and trazodone. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 86
d. Tricyclic antidepressants. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 86
e. Monoamine oxidase inhibitors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 87
2. Electroconvulsive therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 87
3. Transcranial magnetic stimulation . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 89
4. Vagus nerve stimulation . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 90
5. Complementary and alternative treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 91
a. St. John’s wort . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 91
b. S-adenosyl methionine . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 91
c. Omega-3 fatty acids . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 92
d. Folate. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 92
e. Light therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 92
f. Acupuncture. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 92
Specific Psychotherapies . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 93
1. Cognitive and behavioral therapies . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 93
a. Cognitive-behavioral therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 93
b. Behavior therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 94
2. Interpersonal therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 94
3. Psychodynamic psychotherapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 94
4. Marital therapy and family therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 95
5. Problem-solving therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 95
6. Group therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 95
Psychotherapy Combined With Pharmacotherapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 96
Lack of Response to Pharmacotherapy in the Acute Phase . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 97
1. Maximizing initial treatments. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 97
2. Changing to other treatments. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 97
3. Augmenting and combining treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 98
Continuation Treatment . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 98
Maintenance Treatment . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 99
PART C: FUTURE RESEARCH NEEDS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 100
APPENDIX: EDUCATIONAL RESOURCES FOR PATIENTS AND FAMILIES . . . . . . . . . . . . . . . . . . . . . 101
INDIVIDUALS AND ORGANIZATIONS THAT SUBMITTED COMMENTS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 102
ACKNOWLEDGMENT . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 103
REFERENCES . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 103
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
STATEMENT OF INTENT
The APA Practice Guidelines are not intended to be construed or to serve as a standard of medical care. Standards of
medical care are determined on the basis of all clinical data
available for an individual patient and are subject to change
as scientific knowledge and technology advance and practice
patterns evolve. These parameters of practice should be considered guidelines only. Adherence to them will not ensure
a successful outcome for every individual, nor should they
be interpreted as including all proper methods of care or
excluding other acceptable methods of care aimed at the
same results. The ultimate recommendation regarding a
particular clinical procedure or treatment plan must be
made by the psychiatrist in light of the clinical data, the psychiatric evaluation, and the diagnostic and treatment options available. Such recommendations should incorporate
the patient’s personal and sociocultural preferences and values in order to enhance the therapeutic alliance, adherence
to treatment, and treatment outcomes.
This practice guideline was approved in May 2010 and
published in October 2010.
OVERVIEW OF GUIDELINE
DEVELOPMENT PROCESS
This practice guideline was developed under the direction
of the Steering Committee on Practice Guidelines. The
development process is detailed in a document entitled
“APA Guideline Development Process,” which is available from the APA Department of Quality Improvement
and Psychiatric Services. Key features of this process include the following:
• A comprehensive literature review to identify all relevant randomized clinical trials as well as less rigorously
designed clinical trials and case series when evidence
from randomized trials was unavailable
• Development of evidence tables that reviewed the key
features of each identified study, including funding
source, study design, sample sizes, subject characteristics, treatment characteristics, and treatment outcomes
• Initial drafting of the guideline by a work group (“Work
Group”) that included psychiatrists with clinical and research expertise in major depressive disorder
• Production of multiple revised drafts with widespread
review; 15 organizations and 71 individuals submitted
comments.
• Review of the final draft by an Independent Review
Panel of experts with no relationships with industry,
11
who were charged to evaluate the guideline recommendations for bias from potential conflicts of interest.
• Approval by the APA Assembly and Board of Trustees.
• Planned revisions at regular intervals.
Development of this APA practice guideline was not financially supported by any commercial organization. In
addition, the integrity of the guideline has been ensured
by the following mechanisms:
1. Work Group members were selected on the basis of
their expertise and integrity, and they agreed to disclose all potential conflicts of interest before and during
their work on this guideline to the Steering Committee on Practice Guidelines and to each other. Employees of industry were not included on the group, and
the group was balanced to include some persons with
minimal industry relationships. As disclosed on pages
2–3, from initiation of work in 2005 to approval of the
guideline in 2010, some members of the Work Group
on Major Depressive Disorder had relationships with
industry for which they received research grants or income from consulting or speaking related to treatments discussed in the guideline.
2. Iterative guideline drafts were broadly circulated to and
reviewed by the Steering Committee, other experts, allied organizations, and the APA membership; reviewers were asked to disclose their own potential conflicts
of interest relevant to evaluating their comments. Over
1,000 comments were received and were addressed by
substantive revisions by the Work Group. Oversight of
the draft review and revision process was provided by
the chair and vice-chair of the Steering Committee and
by the Medical Editor, none of whom had relationships
with industry.
3. In response to a 2009 report by the Institute of Medicine (1), which advocated that professional organizations that develop and disseminate practice guidelines
should adopt a new policy that members of guideline
work groups have no significant relationships with industry, the following process was implemented: An
independent review panel of experts (“Independent
Review Panel”) having no current relationships with
industry also reviewed the guideline and was charged
with identifying any possible bias. The Independent
Review Panel found no evidence of bias.
The Work Group and the Steering Committee differed on how to rate the strength of recommendation for
psychodynamic psychotherapy. Based on their review of
the available empirical evidence on the use of psycho-
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12
dynamic psychotherapy in individuals with major depressive disorder, the Work Group gave this treatment a level
III rating, i.e., “may be recommended on the basis of individual circumstances.” The Steering Committee gave a
level II rating, “recommended with moderate clinical confidence,” based on the long history of clinical experience
with psychodynamic psychotherapy as well as findings
from several studies of patients who had depressive symptoms but not major depressive disorder per se.
Relevant updates to the literature were identified through
a MEDLINE literature search for articles published since
the second edition of the guideline, published in 2000. For
this edition of the guideline, literature was identified
through a computerized search of MEDLINE, using PubMed, for the period from January 1999 to December 2006.
Using the MeSH headings depression or depressive disorder, as well as the key words major depression, major depressive disorder, neurotic depression, neurotic depressive,
dysthymia, dysthymic, dysthymic disorder, endogenous depression, endogenous depressive, melancholia, melancholic, psychotic depression, atypical depression, seasonal
depression, postpartum depression, postpartum depressive
symptoms, unipolar depression, unipolar depressive, or
pseudodementia yielded 39,157 citations. An additional
8,272 citations were identified by using the key words depression or depressive in combination with the MeSH
headings affective disorders or psychotic or the key words
psychosis, psychotic, catatonic, catatonia, mood disorder,
mood disorders, affective disorder, or affective disorders.
These citations were limited to English language articles
on human treatments using the MeSH headings central
nervous system stimulants, hypnotics and sedatives, anticonvulsants, tranquilizing agents, electric stimulation therapy, electroconvulsive therapy, psychotherapy, antidepressive agents, and monoamine oxidase inhibitors or the key
words antidepressant, antidepressants, antidepressive, antidepressive agents, antidepressive agents, second generation, antidepressive agents tricyclic, antidepressive agents,
tricyclic, fluoxetine, citalopram, escitalopram, paroxetine,
sertraline, venlafaxine, duloxetine, mirtazapine, nefazodone, trazodone, imipramine, desipramine, nortriptyline,
protriptyline, doxepin, trimipramine, amitriptyline, phenelzine, tranylcypromine, isocarboxazid, moclobemide,
antipsychotic agents, testosterone, thyroid, tri iodothyronine, thyroxine, omega 3, s adenosyl methionine, s adenosylmethionine, St. John’s wort, hypericum, selegiline, anticonvulsant, anticonvulsants, antipsychotic, antipsychotic
agent, antianxiety, anti anxiety, benzodiazepine, benzodiazepines, zolpidem, sedative, sedatives, hypnotic, hypnotics,
zaleplon, eszopiclone, valproate, valproic acid, divalproex,
carbamazepine, oxcarbazepine, gabapentin, topiramate,
lamotrigine, lithium, modafinil, methylphenidate, Adder-
APA PRACTICE GUIDELINES
all, amphetamine, amphetamines, dextroamphetamine,
atomoxetine, electroconvulsive, vagal nerve stimulation,
vagus nerve stimulation, VNS, rTMS, rapid transcranial
magnetic, repetitive transcranial magnetic stimulation,
magnetic stimulation, deep brain stimulation, psychotherapy, psychotherapeutic, psychotherapies, behavior therapy,
behaviour therapy, cognitive therapy, cognitive behavior
therapy, cognitive behavioral analysis system, cognitive behavioral therapy, cognitive behaviour therapy, cognitive
behavioural therapy, psychoanalytic, interpersonal therapy,
interpersonal psychotherapy, group therapy, family therapy, marital therapy, couples therapy, psychoanalysis, psychodynamic, aversive therapy, desensitization, exposure
therapy, relaxation techniques, or progressive muscle relaxation. This yielded 13,506 abstracts, which were screened
for relevance with a very modest threshold for inclusion,
then reviewed by the Work Group.
The Psychoanalytic Electronic Publishing database
(http://www.p-e-p.org) was also searched using the terms
major depression or major depressive. This search yielded
112 references. The Cochrane databases were also searched
for the key word depression, and 168 meta-analyses were
identified. Additional, less formal, literature searches were
conducted by APA staff and individual Work Group members and included references through May 2009. Sources
of funding were considered when the Work Group reviewed the literature.
The broad scope of this guideline and the substantial
evidence base resulted in some practical tradeoffs. One
such tradeoff worth highlighting is the decision to build
upon literature reviews of the first and second editions of
the guideline, rather than re-do them. This decision is acknowledged to have resulted in an emphasis of study in
this guideline on newer treatments, because the majority
of studies about older treatments, including tricyclic antidepressants and monoamine oxidase inhibitors, were published in decades prior to 1999. Readers are advised that
the reviews of this older literature are described in the
previous editions of the guideline. The Work Group for
this edition considered the previous editions during their
evidence review, but for practical reasons, that effort is less
well documented than the group’s analysis of the newer
literature. The treatment recommendations of this guideline, however, were developed to reflect the complete evidence base.
This document represents a synthesis of current scientific knowledge and rational clinical practice regarding
the treatment of patients with major depressive disorder.
It strives to be as free as possible of bias toward any theoretical approach to treatment. In order for the reader to
appreciate the evidence base behind the guideline recommendations and the weight that should be given to each
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
recommendation, the summary of treatment recommendations is keyed according to the level of confidence with
which each recommendation is made. Each rating of clinical confidence considers the strength of the available evidence. When evidence from randomized controlled trials
and meta-analyses is limited, the level of confidence may
also incorporate other clinical trials and case reports as well
as clinical consensus with regard to a particular clinical
decision. In the listing of cited references, each reference
is followed by a letter code in brackets that indicates the
nature of the supporting evidence.
GUIDE TO USING THIS
PRACTICE GUIDELINE
The Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition, consists of three parts
(Parts A, B, and C) and many sections, not all of which will
be equally useful for all readers. The following guide is
designed to help readers find the sections that will be most
useful to them.
Part A, “Treatment Recommendations,” is published
as a supplement to the American Journal of Psychiatry and
contains general and specific treatment recommendations. Section I summarizes the key recommendations of
the guideline and codes each recommendation according
to the degree of clinical confidence with which the recommendation is made. Section II is a guide to the formulation and implementation of a treatment plan for the
individual patient. Section III, “Specific Clinical Features
Influencing the Treatment Plan,” discusses a range of clinical considerations that could alter the general recommendations discussed in Section I.
Part B, “Background Information and Review of Available Evidence,” and Part C, “Future Research Needs,” are
not included in the American Journal of Psychiatry supplement but are provided with Part A in the complete guideline, which is available in print format from American
Psychiatric Publishing, Inc., and online through the American Psychiatric Association (http://www.psychiatryonline.com). Part B provides an overview of major depressive
disorder, including general information on natural history,
course, and epidemiology. It also provides a structured
review and synthesis of the evidence that underlies the
recommendations made in Part A. Part C draws from the
previous sections and summarizes areas for which more
research data are needed to guide clinical decisions.
13
To share feedback on this or other published APA
practice guidelines, a form is available at
http://mx.psych.org/survey/reviewform.cfm.
OFF-LABEL USE OF
MEDICATIONS
Medications discussed in this practice guideline may not
have an indication from the U.S. Food and Drug Administration for the disorder or condition for which they are
recommended. Off-label use of medications by individual
physicians is permitted and common. Decisions about offlabel use can be guided by the evidence provided in the
APA practice guideline, other scientific literature, and clinical experience.
INTRODUCTION
This guideline summarizes the specific approaches to
treatment of individuals with major depressive disorder. It
presupposes that the psychiatrist has diagnosed major depressive disorder, according to the criteria defined in
DSM-IV-TR, in an adult patient and has evaluated the
patient to identify general medical conditions that may
contribute to the disease process (e.g., hypothyroidism,
pancreatic carcinoma) or complicate its treatment (e.g.,
cardiac disorders). The treatment recommendations that
follow may also have some relevance for patients who
have depressive symptoms on the basis of other syndromes, such as dysthymic disorder. Because many patients have co-occurring psychiatric disorders, including
substance use disorders, the psychiatrist should also consider applicable treatment guidelines for these diagnoses.
When patients experience depressive symptoms in the
context of another disorder and do not meet the diagnostic criteria for major depressive disorder, the APA practice
guideline pertaining to the primary diagnosis should be
consulted. For patients found to have depressive symptoms within the context of bipolar disorder, the psychiatrist
should refer to APA’s Practice Guideline for the Treatment of
Patients With Bipolar Disorder (2). Recommendations on
the treatment of depressive disorders in children and adolescents can be found in the American Academy of Child
and Adolescent Psychiatry’s Practice Parameter for the Assessment and Treatment of Children and Adolescents With
Depressive Disorders (3).
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
Part A
TREATMENT RECOMMENDATIONS
I.
EXECUTIVE SUMMARY
A. CODING SYSTEM
chiatric history, including identification of past symptoms
of mania, hypomania, or mixed episodes and responses to
previous treatments; a general medical history; a personal
history including information about psychological development and responses to life transitions and major life events;
a social, occupational, and family history (including mood
disorders and suicide); review of the patient’s prescribed
and over-the-counter medications; a review of systems; a
mental status examination; a physical examination; and appropriate diagnostic tests as indicated to rule out possible
general medical causes of depressive symptoms [I]. Assessment of substance use should evaluate past and current use
of illicit drugs and other substances that may trigger or exacerbate depressive symptoms [I].
Each recommendation is identified as falling into one of
three categories of endorsement, indicated by a bracketed
Roman numeral following the statement. The three categories represent varying levels of clinical confidence:
[I] Recommended with substantial clinical confidence
[II] Recommended with moderate clinical confidence
[III] May be recommended on the basis of individual circumstances
B. SUMMARY OF RECOMMENDATIONS
1. Psychiatric management
Psychiatric management consists of a broad array of interventions and activities that psychiatrists should initiate
and continue to provide to patients with major depressive
disorder through all phases of treatment [I].
c.
Evaluate the safety of the patient
A careful and ongoing evaluation of suicide risk is necessary for all patients with major depressive disorder [I].
Such an assessment includes specific inquiry about suicidal thoughts, intent, plans, means, and behaviors; identification of specific psychiatric symptoms (e.g., psychosis,
severe anxiety, substance use) or general medical conditions that may increase the likelihood of acting on suicidal
ideas; assessment of past and, particularly, recent suicidal
behavior; delineation of current stressors and potential
protective factors (e.g., positive reasons for living, strong
social support); and identification of any family history of
suicide or mental illness [I]. In addition to assessing suicide risk per se, it is important to assess the patient’s level
of self-care, hydration, and nutrition, each of which can be
compromised by severe depressive symptoms [I]. As part
of the assessment process, impulsivity and potential for
risk to others should also be evaluated, including any history of violence or violent or homicidal ideas, plans, or intentions [I]. An evaluation of the impact of the depression
on the patient’s ability to care for dependents is an important component of the safety evaluation [I]. The patient’s
risk of harm to him- or herself and to others should also be
monitored as treatment proceeds [I].
a. Establish and maintain a therapeutic alliance
In establishing and maintaining a therapeutic alliance, it is
important to collaborate with the patient in decision making and attend to the patient’s preferences and concerns
about treatment [I]. Management of the therapeutic alliance should include awareness of transference and countertransference issues, even if these are not directly addressed
in treatment [II]. Severe or persistent problems of poor alliance or nonadherence to treatment may be caused by the
depressive symptoms themselves or may represent psychological conflicts or psychopathology for which psychotherapy should be considered [II].
b. Complete the psychiatric assessment
Patients should receive a thorough diagnostic assessment in
order to establish the diagnosis of major depressive disorder, identify other psychiatric or general medical conditions
that may require attention, and develop a comprehensive
plan for treatment [I]. This evaluation generally includes a
history of the present illness and current symptoms; a psy-
15
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16
d. Establish the appropriate setting for treatment
The psychiatrist should determine the least restrictive
setting for treatment that will be most likely not only to
address the patient’s safety, but also to promote improvement in the patient’s condition [I]. The determination of
an appropriate setting for treatment should include consideration of the patient’s symptom severity, co-occurring
psychiatric or general medical conditions, available support
system, and level of functioning [I]. The determination of a
treatment setting should also include consideration of the
patient’s ability to adequately care for him- or herself, to
provide reliable feedback to the psychiatrist, and to cooperate with treatment of the major depressive disorder [I].
Measures such as hospitalization should be considered for
patients who pose a serious threat of harm to themselves
or others [I]. Patients who refuse inpatient treatment can
be hospitalized involuntarily if their condition meets the
criteria of the local jurisdiction for involuntary admission
[I]. Admission to a hospital or, if available, an intensive day
program, may also be indicated for severely ill patients who
lack adequate social support outside of a hospital setting,
who have complicating psychiatric or general medical
conditions, or who have not responded adequately to outpatient treatment [I]. The optimal treatment setting and
the patient’s likelihood of benefit from a different level of
care should be reevaluated on an ongoing basis throughout the course of treatment [I].
e. Evaluate functional impairment and quality of life
Major depressive disorder can alter functioning in numerous spheres of life including work, school, family, social
relationships, leisure activities, or maintenance of health
and hygiene. The psychiatrist should evaluate the patient’s
activity in each of these domains and determine the presence, type, severity, and chronicity of any dysfunction [I].
In developing a treatment plan, interventions should be
aimed at maximizing the patient’s level of functioning as
well as helping the patient to set specific goals appropriate
to his or her functional impairments and symptom severity [I].
f. Coordinate the patient’s care with other clinicians
Many patients with major depressive disorder will be evaluated by or receive treatment from other health care professionals in addition to the psychiatrist. If more than one
clinician is involved in providing the care, all treating clinicians should have sufficient ongoing contact with the
patient and with each other to ensure that care is coordinated, relevant information is available to guide treatment
decisions, and treatments are synchronized [I].
In ruling out general medical causes of depressive symptoms, it is important to ensure that a general medical eval-
APA PRACTICE GUIDELINES
uation has been done [I], either by the psychiatrist or by
another health care professional. Extensive or specialized
testing for general medical causes of depressive symptoms
may be conducted based on individual characteristics of
the patient [III].
g. Monitor the patient’s psychiatric status
The patient’s response to treatment should be carefully
monitored [I]. Continued monitoring of co-occurring
psychiatric and/or medical conditions is also essential to
developing and refining a treatment plan for an individual
patient [I].
h. Integrate measurements into psychiatric management
Tailoring the treatment plan to match the needs of the
particular patient requires a careful and systematic assessment of the type, frequency, and magnitude of psychiatric
symptoms as well as ongoing determination of the therapeutic benefits and side effects of treatment [I]. Such assessments can be facilitated by integrating clinician- and/or
patient-administered rating scale measurements into initial and ongoing evaluation [II].
i. Enhance treatment adherence
The psychiatrist should assess and acknowledge potential
barriers to treatment adherence (e.g., lack of motivation
or excessive pessimism due to depression; side effects of
treatment; problems in the therapeutic relationship; logistical, economic, or cultural barriers to treatment) and
collaborate with the patient (and if possible, the family) to
minimize the impact of these potential barriers [I]. In addition, the psychiatrist should encourage patients to articulate any fears or concerns about treatment or its side effects
[I]. Patients should be given a realistic notion of what can
be expected during the different phases of treatment, including the likely time course of symptom response and
the importance of adherence for successful treatment and
prophylaxis [I].
j. Provide education to the patient and the family
Education about the symptoms and treatment of major
depressive disorder should be provided in language that is
readily understandable to the patient [I]. With the patient’s permission, family members and others involved in
the patient’s day-to-day life may also benefit from education about the illness, its effects on functioning (including
family and other interpersonal relationships), and its treatment [I]. Common misperceptions about antidepressants
(e.g., they are addictive) should be clarified [I]. In addition,
education about major depressive disorder should address
the need for a full acute course of treatment, the risk of relapse, the early recognition of recurrent symptoms, and the
need to seek treatment as early as possible to reduce the risk
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
of complications or a full-blown episode of major depression [I]. Patients should also be told about the need to
taper antidepressants, rather than discontinuing them
precipitously, to minimize the risk of withdrawal symptoms or symptom recurrence [I]. Patient education also
includes general promotion of healthy behaviors such as
exercise, good sleep hygiene, good nutrition, and decreased
use of tobacco, alcohol, and other potentially deleterious
substances [I]. Educational tools such as books, pamphlets,
and trusted web sites can augment the face-to-face education provided by the clinician [I].
2. Acute phase
a. Choice of an initial treatment modality
Treatment in the acute phase should be aimed at inducing
remission of the major depressive episode and achieving a
full return to the patient’s baseline level of functioning [I].
Acute phase treatment may include pharmacotherapy, depression-focused psychotherapy, the combination of medications and psychotherapy, or other somatic therapies
such as electroconvulsive therapy (ECT), transcranial magnetic stimulation (TMS), or light therapy, as described in the
sections that follow. Selection of an initial treatment modality should be influenced by clinical features (e.g., severity of symptoms, presence of co-occurring disorders
or psychosocial stressors) as well as other factors (e.g., patient preference, prior treatment experiences) [I]. Any
treatment should be integrated with psychiatric management and any other treatments being provided for other
diagnoses [I].
1. Pharmacotherapy
An antidepressant medication is recommended as an initial treatment choice for patients with mild to moderate
major depressive disorder [I] and definitely should be provided for those with severe major depressive disorder unless ECT is planned [I]. Because the effectiveness of antidepressant medications is generally comparable between
classes and within classes of medications, the initial selection of an antidepressant medication will largely be based
on the anticipated side effects, the safety or tolerability of
these side effects for the individual patient, pharmacological properties of the medication (e.g., half-life, actions on
cytochrome P450 enzymes, other drug interactions), and additional factors such as medication response in prior episodes, cost, and patient preference [I]. For most patients, a
selective serotonin reuptake inhibitor (SSRI), serotonin
norepinephrine reuptake inhibitor (SNRI), mirtazapine,
or bupropion is optimal [I]. In general, the use of nonselective monoamine oxidase inhibitors (MAOIs) (e.g., phenelzine, tranylcypromine, isocarboxazid) should be restricted
17
to patients who do not respond to other treatments [I],
given the necessity for dietary restrictions with these medications and the potential for deleterious drug-drug interactions. In patients who prefer complementary and alternative therapies, S-adenosyl methionine (SAMe) [III] or
St. John’s wort [III] might be considered, although evidence
for their efficacy is modest at best, and careful attention to
drug-drug interactions is needed with St. John’s wort [I].
Once an antidepressant medication has been initiated,
the rate at which it is titrated to a full therapeutic dose
should depend upon the patient’s age, the treatment setting, and the presence of co-occurring illnesses, concomitant pharmacotherapy, or medication side effects [I].
During the acute phase of treatment, patients should be
carefully and systematically monitored on a regular basis
to assess their response to pharmacotherapy, identify the
emergence of side effects (e.g., gastrointestinal symptoms,
sedation, insomnia, activation, changes in weight, and cardiovascular, neurological, anticholinergic, or sexual side effects), and assess patient safety [I]. The frequency of patient
monitoring should be determined based upon the patient’s
symptom severity (including suicidal ideas), co-occurring
disorders (including general medical conditions), cooperation with treatment, availability of social supports, and the
frequency and severity of side effects with the chosen treatment [II]. If antidepressant side effects do occur, an initial
strategy is to lower the dose of the antidepressant or to
change to an antidepressant that is not associated with
that side effect [I].
2. Other somatic therapies
ECT is recommended as a treatment of choice for patients with severe major depressive disorder that is not responsive to psychotherapeutic and/or pharmacological
interventions, particularly in those who have significant
functional impairment or have not responded to numerous medication trials [I]. ECT is also recommended for
individuals with major depressive disorder who have associated psychotic or catatonic features [I], for those with an
urgent need for response (e.g., patients who are suicidal
or nutritionally compromised due to refusal of food or fluids) [I], and for those who prefer ECT or have had a previous positive response to ECT [II].
Bright light therapy might be used to treat seasonal affective disorder as well as nonseasonal depression [III].
3. Psychotherapy
Use of a depression-focused psychotherapy alone is recommended as an initial treatment choice for patients with
mild to moderate major depressive disorder [I], with clinical evidence supporting the use of cognitive-behavioral
therapy (CBT) [I], interpersonal psychotherapy [I], psy-
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18
chodynamic therapy [II], and problem-solving therapy
[III] in individual [I] and in group [III] formats. Factors
that may suggest the use of psychotherapeutic interventions include the presence of significant psychosocial
stressors, intrapsychic conflict, interpersonal difficulties,
a co-occurring axis II disorder, treatment availability, or—
most important—patient preference [II]. In women who
are pregnant, wish to become pregnant, or are breastfeeding, a depression-focused psychotherapy alone is recommended [II] and depending on the severity of symptoms,
should be considered as an initial option [I]. Considerations in the choice of a specific type of psychotherapy include the goals of treatment (in addition to resolving major
depressive symptoms), prior positive response to a specific
type of psychotherapy, patient preference, and the availability of clinicians skilled in the specific psychotherapeutic approach [II]. As with patients who are receiving pharmacotherapy, patients receiving psychotherapy should be
carefully and systematically monitored on a regular basis to
assess their response to treatment and assess patient safety
[I]. When determining the frequency of psychotherapy
sessions for an individual patient, the psychiatrist should
consider multiple factors, including the specific type and
goals of psychotherapy, symptom severity (including suicidal ideas), co-occurring disorders, cooperation with treatment, availability of social supports, and the frequency of
visits necessary to create and maintain a therapeutic relationship, ensure treatment adherence, and monitor and address depressive symptoms and suicide risk [II]. Marital and
family problems are common in the course of major depressive disorder, and such problems should be identified
and addressed, using marital or family therapy when indicated [II].
4. Psychotherapy plus antidepressant medication
The combination of psychotherapy and antidepressant
medication may be used as an initial treatment for patients
with moderate to severe major depressive disorder [I]. In
addition, combining psychotherapy and medication may
be a useful initial treatment even in milder cases for patients with psychosocial or interpersonal problems, intrapsychic conflict, or co-occurring Axis II disorder [II]. In
general, when choosing an antidepressant or psychotherapeutic approach for combination treatment, the same issues should be considered as when selecting a medication
or psychotherapy for use alone [I].
b. Assessing the adequacy of treatment response
In assessing the adequacy of a therapeutic intervention, it
is important to establish that treatment has been administered for a sufficient duration and at a sufficient frequency or,
in the case of medication, dose [I]. Onset of benefit from
APA PRACTICE GUIDELINES
psychotherapy tends to be a bit more gradual than that
from medication, but no treatment should continue unmodified if there has been no symptomatic improvement
after 1 month [I]. Generally, 4–8 weeks of treatment are
needed before concluding that a patient is partially responsive or unresponsive to a specific intervention [II].
c. Strategies to address nonresponse
For individuals who have not responded fully to treatment, the acute phase of treatment should not be concluded prematurely [I], as an incomplete response to
treatment is often associated with poor functional outcomes. If at least a moderate improvement in symptoms
is not observed within 4–8 weeks of treatment initiation,
the diagnosis should be reappraised, side effects assessed,
complicating co-occurring conditions and psychosocial
factors reviewed, and the treatment plan adjusted [I]. It is
also important to assess the quality of the therapeutic alliance and treatment adherence [I]. For patients in psychotherapy, additional factors to be assessed include the
frequency of sessions and whether the specific approach
to psychotherapy is adequately addressing the patient’s
needs [I]. If medications are prescribed, the psychiatrist
should determine whether pharmacokinetic [I] or pharmacodynamic [III] factors suggest a need to adjust medication doses. With some TCAs, a drug blood level can
help determine if additional dose adjustments are required [I].
After an additional 4–8 weeks of treatment, if the patient continues to show minimal or no improvement in
symptoms, the psychiatrist should conduct another thorough review of possible contributory factors and make additional changes in the treatment plan [I]. Consultation
should also be considered [II].
A number of strategies are available when a change in
the treatment plan seems necessary. For patients treated
with an antidepressant, optimizing the medication dose is
a reasonable first step if the side effect burden is tolerable
and the upper limit of a medication dose has not been
reached [II]. Particularly for those who have shown minimal improvement or experienced significant medication
side effects, other options include augmenting the antidepressant with a depression-focused psychotherapy [I] or
with other agents [II] or changing to another non-MAOI
antidepressant [I]. Patients may be changed to an antidepressant from the same pharmacological class (e.g., from
one SSRI to another SSRI) or to one from a different class
(e.g., from an SSRI to a tricyclic antidepressant [TCA]) [II].
For patients who have not responded to trials of SSRIs, a
trial of an SNRI may be helpful [II]. Augmentation of antidepressant medications can utilize another non-MAOI
antidepressant [II], generally from a different pharmaco-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
logical class, or a non-antidepressant medication such as
lithium [II], thyroid hormone [II], or a second-generation
antipsychotic [II]. Additional strategies with less evidence
for efficacy include augmentation using an anticonvulsant
[III], omega-3 fatty acids [III], folate [III], or a psychostimulant medication [III], including modafinil [III]. If anxiety
or insomnia are prominent features, consideration can be
given to anxiolytic and sedative-hypnotic medications
[III], including buspirone, benzodiazepines, and selective
γ-aminobutyric acid (GABA) agonist hypnotics (e.g., zolpidem, eszopiclone). For patients whose symptoms have
not responded adequately to medication, ECT remains the
most effective form of therapy and should be considered
[I]. In patients capable of adhering to dietary and medication restrictions, an additional option is changing to a nonselective MAOI [II] after allowing sufficient time between
medications to avoid deleterious interactions [I]. Transdermal selegiline, a relatively selective MAO B inhibitor with
fewer dietary and medication restrictions, or transcranial
magnetic stimulation could also be considered [II]. Vagus
nerve stimulation (VNS) may be an additional option for
individuals who have not responded to at least four adequate trials of antidepressant treatment, including ECT
[III].
For patients treated with psychotherapy, consideration
should be given to increasing the intensity of treatment
or changing the type of therapy [II]. If psychotherapy is
used alone, the possible need for medications in addition
to or in lieu of psychotherapy should be assessed [I]. Patients who have a history of poor treatment adherence or
incomplete response to adequate trials of single treatment modalities may benefit from combined treatment
with medication and a depression-focused psychotherapy
[II].
3. Continuation phase
During the continuation phase of treatment, the patient
should be carefully monitored for signs of possible relapse
[I]. Systematic assessment of symptoms, side effects, adherence, and functional status is essential [I] and may be
facilitated through the use of clinician- and/or patientadministered rating scales [II]. To reduce the risk of relapse, patients who have been treated successfully with
antidepressant medications in the acute phase should continue treatment with these agents for 4–9 months [I]. In
general, the dose used in the acute phase should be used
in the continuation phase [II]. To prevent a relapse of
depression in the continuation phase, depression-focused
psychotherapy is recommended [I], with the best evidence
available for CBT.
19
Patients who respond to an acute course of ECT should
receive continuation pharmacotherapy [I], with the best
evidence available for the combination of lithium and
nortriptyline. Alternatively, patients who have responded
to an acute course of ECT may be given continuation ECT,
particularly if medication or psychotherapy has been ineffective in maintaining remission [II].
4. Maintenance phase
In order to reduce the risk of a recurrent depressive episode, patients who have had three or more prior major depressive episodes or who have chronic major depressive
disorder should proceed to the maintenance phase of treatment after completing the continuation phase [I]. Maintenance therapy should also be considered for patients with
additional risk factors for recurrence, such as the presence
of residual symptoms, ongoing psychosocial stressors, early
age at onset, and family history of mood disorders [II]. Additional considerations that may play a role in the decision
to use maintenance therapy include patient preference, the
type of treatment received, the presence of side effects during continuation therapy, the probability of recurrence, the
frequency and severity of prior depressive episodes (including factors such as psychosis or suicide risk), the persistence
of depressive symptoms after recovery, and the presence of
co-occurring disorders [II]. Such factors also contribute to
decisions about the duration of the maintenance phase [II].
For many patients, particularly for those with chronic and
recurrent major depressive disorder or co-occurring medical and/or psychiatric disorders, some form of maintenance
treatment will be required indefinitely [I].
During the maintenance phase, an antidepressant medication that produced symptom remission during the acute
phase and maintained remission during the continuation
phase should be continued at a full therapeutic dose [II]. If
a depression-focused psychotherapy has been used during
the acute and continuation phases of treatment, maintenance treatment should be considered, with a reduced
frequency of sessions [II]. For patients whose depressive
episodes have not previously responded to acute or continuation treatment with medications or a depressionfocused psychotherapy but who have shown a response to
ECT, maintenance ECT may be considered [III]. Maintenance treatment with VNS is also appropriate for individuals whose symptoms have responded to this treatment
modality [III].
Due to the risk of recurrence, patients should be monitored systematically and at regular intervals during the
maintenance phase [I]. Use of standardized measurement
aids in the early detection of recurrent symptoms [II].
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20
5. Discontinuation of treatment
When pharmacotherapy is being discontinued, it is best
to taper the medication over the course of at least several
weeks [I]. To minimize the likelihood of discontinuation
symptoms, patients should be advised not to stop medications abruptly and to take medications with them when
they travel or are away from home [I]. A slow taper or
temporary change to a longer half-life antidepressant may
reduce the risk of discontinuation syndrome [II] when discontinuing antidepressants or reducing antidepressant
doses. Before the discontinuation of active treatment, patients should be informed of the potential for a depressive
relapse and a plan should be established for seeking treatment in the event of recurrent symptoms [I]. After discontinuation of medications, patients should continue to be
monitored over the next several months and should receive
another course of adequate acute phase treatment if symptoms recur [I].
For patients receiving psychotherapy, it is important to
raise the issue of treatment discontinuation well in advance of the final session [I], although the exact process by
which this occurs will vary with the type of therapy.
6. Clinical factors influencing treatment
a. Psychiatric factors
For suicidal patients, psychiatrists should consider an increased intensity of treatment, including hospitalization
when warranted [I] and/or combined treatment with
pharmacotherapy and psychotherapy [II]. Factors to consider in determining the nature and intensity of treatment
include (but are not limited to) the nature of the doctorpatient alliance, the availability and adequacy of social supports, access to and lethality of suicide means, the presence
of a co-occurring substance use disorder, and past and family history of suicidal behavior [I].
For patients who exhibit psychotic symptoms during
an episode of major depressive disorder, treatment should
include a combination of antipsychotic and antidepressant
medications or ECT [I]. When patients exhibit cognitive
dysfunction during a major depressive episode, they may
have an increased likelihood of future dementia, making it
important to assess cognition in a systematic fashion over
the course of treatment [I].
Catatonic features that occur as part of a major depressive episode should be treated with a benzodiazepine [I] or
barbiturate [II], typically in conjunction with an antidepressant [II]. If catatonic symptoms persist, ECT is recommended [I]. To reduce the likelihood of general medical
complications, patients with catatonia may also require
supportive medical interventions, such as hydration, nutritional support, prophylaxis against deep vein thrombo-
APA PRACTICE GUIDELINES
sis, turning to reduce risks of decubitus ulcers, and passive
range of motion to reduce risk of contractures [I]. If antipsychotic medication is needed, it is important to monitor
for signs of neuroleptic malignant syndrome, to which patients with catatonia may have a heightened sensitivity
[II].
When patients with a major depressive disorder also
have a co-occurring psychiatric illness, the clinician should
address each disorder as part of the treatment plan [I]. Benzodiazepines may be used adjunctively in individuals with
major depressive disorder and co-occurring anxiety [II], although these agents do not treat depressive symptoms, and
careful selection and monitoring is needed in individuals
with co-occurring substance use disorders [I].
In patients who smoke, bupropion [I] or nortriptyline
[II] may be options to simultaneously treat depression and
assist with smoking cessation. When possible, a period of
substance abstinence can help determine whether the depressive episode is related to substance intoxication or
withdrawal [II]. Factors that suggest a need for antidepressant treatment soon after cessation of substance use
include a family history of major depressive disorder and
a history of major depressive disorder preceding the onset of the substance use disorder or during periods of sobriety [II].
For patients who have a personality disorder as well as
major depressive disorder, psychiatrists should institute
treatment for the major depressive disorder [I] and consider psychotherapeutic and adjunctive pharmacotherapeutic treatment for personality disorder symptoms [II].
b. Demographic and psychosocial factors
Several aspects of assessment and treatment differ between women and men. Because the symptoms of some
women may fluctuate with gonadal hormone levels, the
evaluation should include a detailed assessment of mood
changes across the reproductive life history (e.g., menstruation, pregnancy, birth control including oral contraception use, abortions, menopause) [I]. When prescribing
medications to women who are taking oral contraceptives,
the potential effects of drug-drug interactions must be
considered [I]. For women in the perimenopausal period,
SSRI and SNRI antidepressants are useful in ameliorating
depression as well as in reducing somatic symptoms such
as hot flashes [II]. Both men and women who are taking antidepressants should be asked whether sexual side effects
are occurring with these medications [I]. Men for whom
trazodone is prescribed should be warned of the risk of
priapism [I].
The treatment of major depressive disorder in women
who are pregnant or planning to become pregnant requires a careful consideration of the benefits and risks of
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
available treatment options for the patient and the fetus [I].
For women who are currently receiving treatment for depression, a pregnancy should be planned, whenever possible, in consultation with the treating psychiatrist, who
may wish to consult with a specialist in perinatal psychiatry [I]. In women who are pregnant, planning to become
pregnant, or breast-feeding, depression-focused psychotherapy alone is recommended [II] and should always be
considered as an initial option, particularly for mild to
moderate depression, for patients who prefer psychotherapy, or for those with a prior positive response to
psychotherapy [I]. Antidepressant medication should be
considered for pregnant women who have moderate to
severe major depressive disorder as well as for those who
are in remission from major depressive disorder, are receiving maintenance medication, and are deemed to be at
high risk for a recurrence if the medication is discontinued [II]. When antidepressants are prescribed to a pregnant
woman, changes in pharmacokinetics during pregnancy
may require adjustments in medication doses [I]. Electroconvulsive therapy may be considered for the treatment of
depression during pregnancy in patients who have psychotic or catatonic features, whose symptoms are severe
or have not responded to medications, or who prefer treatment with ECT [II]. When a woman decides to nurse, the
potential benefits of antidepressant medications for the
mother should be balanced against the potential risks to
the newborn from receiving antidepressant in the mother’s
milk [I]. For women who are depressed during the postpartum period, it is important to evaluate for the presence
of suicidal ideas, homicidal ideas, and psychotic symptoms [I]. The evaluation should also assess parenting skills
for the newborn and for other children in the patient’s
care [I].
In individuals with late-life depression, identification
of co-occurring general medical conditions is essential, as
these disorders may mimic depression or affect choice or
dosing of medications [I]. Older individuals may also be
particularly sensitive to medication side effects (e.g.,
hypotension, anticholinergic effects) and require adjustment of medication doses for hepatic or renal dysfunction
[I]. In other respects, treatment for depression should parallel that used in younger age groups [I].
The assessment and treatment of major depressive disorder should consider the impact of language barriers, as
well as cultural variables that may influence symptom presentation, treatment preferences, and the degree to which
psychiatric illness is stigmatized [I]. When antidepressants are prescribed, the psychiatrist should recognize
that ethnic groups may differ in their metabolism and response to medications [II].
21
Issues relating to the family situation and family history, including mood disorders and suicide, can also affect
treatment planning and are an important element of the
initial evaluation [I]. A family history of bipolar disorder
or acute psychosis suggests a need for increased attention
to possible signs of bipolar illness in the patient (e.g., with
antidepressant treatment) [I]. A family history of recurrent major depressive disorder increases the likelihood of
recurrent episodes in the patient and supports a need for
maintenance treatment [II]. Family history of a response
to a particular antidepressant may sometimes help in
choosing a specific antidepressant for the patient [III]. Because problems within the family may become an ongoing
stressor that hampers the patient’s response to treatment,
and because depression in a family is a major stress in itself, such factors should be identified and strong consideration given to educating the family about the nature of
the illness, enlisting the family’s support, and providing
family therapy, when indicated [II].
For patients who have experienced a recent bereavement, psychotherapy or antidepressant treatment should
be used when the reaction to a loss is particularly prolonged or accompanied by significant psychopathology
and functional impairment [I]. Support groups may be
helpful for some bereaved individuals [III].
c.
Co-occurring general medical conditions
In patients with major depressive disorder, it is important
to recognize and address the potential interplay between
major depressive disorder and any co-occurring general
medical conditions [I]. Communication with other clinicians who are providing treatment for general medical
conditions is recommended [I]. The clinical assessment
should include identifying any potential interactions between medications used to treat depression and those used
to treat general medical conditions [I]. Assessment of pain
is also important as it can contribute to and co-occur with
depression [I]. In addition, the psychiatrist should consider the effects of prescribed psychotropic medications
on the patient’s general medical conditions, as well as the
effects of interventions for such disorders on the patient’s
psychiatric condition [I].
In patients with preexisting hypertension or cardiac
conditions, treatment with specific antidepressant agents
may suggest a need for monitoring of vital signs or cardiac rhythm (e.g., electrocardiogram [ECG] with TCA
treatment; heart rate and blood pressure assessment with
SNRIs and TCAs) [I]. When using antidepressant medications with anticholinergic side effects, it is important to
consider the potential for increases in heart rate in individuals with cardiac disease, worsening cognition in individ-
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22
APA PRACTICE GUIDELINES
uals with dementia, development of bladder outlet
obstruction in men with prostatic hypertrophy, and precipitation or worsening of narrow angle glaucoma [I]. Some
antidepressant drugs (e.g., bupropion, clomipramine,
maprotiline) reduce the seizure threshold and should be
used with caution in individuals with preexisting seizure disorders [II]. In individuals with Parkinson’s disease, the
choice of an antidepressant should consider that serotonergic agents may worsen symptoms of the disease [II],
that bupropion has potential dopamine agonist effects
(benefitting symptoms of Parkinson’s disease but potentially worsening psychosis) [II], and that selegiline has antiparkinsonian and antidepressant effects but may interact
with L-dopa and with other antidepressant agents [I]. In
treating the depressive syndrome that commonly occurs
following a stroke, consideration should be given to the
potential for interactions between antidepressants and
anticoagulating (including antiplatelet) medications [I].
Given the health risks associated with obesity and the tendency of some antidepressant medications to contribute to
weight gain, longitudinal monitoring of weight (either by
direct measurement or patient report) is recommended
[I], as well as calculation of body mass index (BMI) [II]. If
significant increases are noted in the patient’s weight or
BMI, the clinician and patient should discuss potential approaches to weight control such as diet, exercise, change in
medication, nutrition consultation, or collaboration with
the patient’s primary care physician [I]. In patients who
have undergone bariatric surgery to treat obesity, adjustment of medication formulations or doses may be required because of altered medication absorption [I]. For
diabetic patients, it is useful to collaborate with the patient’s primary care physician in monitoring diabetic control when initiating antidepressant therapy or making
significant dosing adjustments [II]. Clinicians should be
alert to the possibility of sleep apnea in patients with depres-
II.
sion, particularly those who present with daytime sleepiness, fatigue, or treatment-resistant symptoms [II]. In
patients with known sleep apnea, treatment choice should
consider the sedative side effects of medication, with minimally sedating options chosen whenever possible [I]. Given
the significant numbers of individuals with unrecognized
human immunodeficiency virus (HIV) infection and the
availability of effective treatment, consideration should be
given to HIV risk assessment and screening [I]. For patients with HIV infection who are receiving antiretroviral
therapy, the potential for drug-drug interactions needs to be
assessed before initiating any psychotropic medications [I].
Patients who are being treated with antiretroviral medications should be cautioned about drug-drug interactions
with St. John’s wort that can reduce the effectiveness of
HIV treatments [I]. In patients with hepatitis C infection,
interferon can exacerbate depressive symptoms, making
it important to monitor patients carefully for worsening
depressive symptoms during the course of interferon
treatment [I]. Because tamoxifen requires active 2D6 enzyme function to be clinically efficacious, patients who
receive tamoxifen for breast cancer or other indications
should generally be treated with an antidepressant (e.g.,
citalopram, escitalopram, venlafaxine, desvenlafaxine)
that has minimal effect on metabolism through the cytochrome P450 2D6 isoenzyme [I]. When depression occurs in the context of chronic pain, SNRIs and TCAs may
be preferable to other antidepressive agents [II]. When
ECT is used to treat major depressive disorder in an individual with a co-occurring general medical condition,
the evaluation should identify conditions that could require modifications in ECT technique (e.g., cardiac conditions, hypertension, central nervous system lesions) [I];
these should be addressed insofar as possible and discussed with the patient as part of the informed consent
process [I].
FORMULATION AND IMPLEMENTATION
OF A TREATMENT PLAN
A. PSYCHIATRIC MANAGEMENT
For all patients with major depressive disorder, psychiatric management includes a broad array of possible interventions and activities. Essential components include
educating the patient and when appropriate the family
about depression, discussing treatment options and interventions, and enhancing adherence to treatment. Devel-
oping a successful plan of treatment for individuals with
major depressive disorder is also promoted by an initial,
thorough assessment of the patient. In addition, the psychiatrist must determine the treatment setting that will be
most likely to enhance the patient’s safety as well as promote improvement in the patient’s condition. These elements of psychiatric management are described in more
detail below.
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
1. Establish and maintain a therapeutic alliance
A psychiatric assessment begins with establishing therapeutic rapport and developing an alliance with the patient,
regardless of the treatment modalities ultimately selected.
The alliance itself may be the primary active therapeutic
agent even for patients who receive monotherapy with
medication (4). To establish and maintain a therapeutic alliance, it is important for the psychiatrist to be sensitive to
the patient’s concerns. By virtue of their depressed state,
patients often view themselves in a negative light. They
may feel unworthy of help, embarrassed or ashamed of
having an illness, guilty about placing burdens on family
members or the clinician, and distant or alienated from
others. Individuals may also have a negative view of prior
treatment experiences or have misconceptions about psychiatric treatment, which can color the therapeutic relationship. Such issues require open discussion to educate
the patient about the goals and framework of treatment
and to provide an empathic and trusting environment in
which the patient feels comfortable expressing his or her
self-doubts, fears, and other concerns. Cultural and religious factors may influence the patient’s view of the depressive illness, his or her receptiveness to psychiatric treatment,
and his or her preference of treatment modalities (5–7).
Establishing a therapeutic alliance with a clinician of a different background may present additional challenges for
some patients. Management of the therapeutic alliance
should also include awareness of transference and countertransference issues, even if these are not directly addressed
in treatment.
Because patients frequently have strong preferences
about treatment options, the psychiatrist should identify
the patient’s wishes for treatment and collaborate with the
patient in choosing among effective treatments. In addition, treatment adherence can be enhanced by the delivery
of patient-centered care and by a strong treatment alliance with the psychiatrist. Severe or persistent problems
of poor alliance or nonadherence to treatment may be
caused by the depressive symptoms themselves. They may
also represent psychological conflicts or a psychopathological condition for which psychotherapy should be considered.
If possible and appropriate, the family should be included in discussions about the patient’s illness and plans
for treatment. When family members are involved, they
can also be encouraged to play a helpful role in improving
the patient’s adherence to treatment and supporting the
therapeutic alliance.
2. Complete the psychiatric assessment
Patients with symptoms of depression should receive a
thorough biopsychosocial assessment, both to determine
23
whether a diagnosis of major depressive disorder is warranted and to identify the presence of other psychiatric or
general medical conditions. The general principles and
components of a complete psychiatric evaluation have been
outlined in APA’s Practice Guideline for Psychiatric Evaluation of Adults, Second Edition (8). The evaluation includes a
history of the present illness and current symptoms, including vegetative symptoms and symptoms of mania or
psychosis, as well as a psychiatric history that particularly
notes current treatments, responses to previous treatments, past hospitalizations or suicide attempts, and the
presence of co-occurring psychiatric disorders. Assessing
the severity of the specific symptoms of depression may
be aided by the use of standardized clinician- or patientadministered rating scales such as those described in Section II.A.8.
Many individuals with depression attempt to alleviate
symptoms through the use of alternative or complementary treatments, over-the-counter or prescription medications or dietary regimens, or through use of caffeine,
tobacco, alcohol, or other substances, which may precipitate or exacerbate depressive symptoms. Consequently,
each of these factors should be carefully assessed. The personal history will include an assessment of psychological
development; a sexual history, including history of sexual
abuse or assault; identification of early life trauma, including physical, sexual, or emotional abuse or neglect; determination of responses to life transitions, major life events,
or significant traumas; a social history; and an occupational
history, including history of military service. Co-occurring general medical conditions are common and can influence the diagnosis of major depressive disorder as well
as choices of treatment. Thus, a general medical history is
essential, along with a review of the patient’s current medications; a review of systems, including assessment for
pain; and any indicated diagnostic tests or physical examinations. The latter may be done by the psychiatrist or by
another physician or medically trained clinician. A mental
status examination is crucial in identifying signs of depression, associated psychosis, cognitive deficits, and factors
influencing suicide risk (e.g., suicidal ideas, anxiety), as
well as in identifying co-occurring psychiatric disorders.
Because major depressive disorder is associated with functional impairment, the presence, type, and severity of the
dysfunction should be evaluated. Impairments can include
deficits in interpersonal relationships and family functioning, work performance, maintenance of health and
hygiene, and deficits in quality of life. Whenever feasible,
assessment should also include input from family members
in order to determine the impact of the patient’s condition
on his or her family. Family members and significant others can also report key elements of the patient’s history or
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24
recent status that the patient may minimize or be unable
to recall or report accurately. In addition, family functioning may affect the outcome of the patient’s depressive illness (9, 10).
A family history is also important to obtain and involves the collection of the family pedigree including parents, grandparents, and number and sex of siblings and
children. For patients with children at home, information
on their symptom state may be useful because of the high
possibility of psychiatric problems in the offspring of a depressed parent (11, 12). Such problems may require intervention or may be an added stressor for the patient. The
family history includes history of depression or other mood
disorders, substance use disorders, psychosis, suicide, and
unusual behaviors in the patient’s relatives along with any
associated impairments. Because family history is a potent
and consistent risk factor for mental disorders, formulating diagnosis and treatment decisions for the patient can
be aided by knowing the age of onset and severity of psychiatric symptoms in the patient’s family, as well as relatives’
psychiatric treatment history, especially the tolerability
and effectiveness of those treatments.
In establishing a diagnosis of major depressive disorder
as part of the initial assessment, other differential diagnostic possibilities are important to consider. An initial
consideration in the differential diagnosis is mood disorder
due to a general medical condition. Specific medical conditions that are important to consider and that may be associated with a major depressive episode include neurological
conditions (e.g., stroke, Parkinson’s disease, dementia,
multiple sclerosis), thyroid disorders, metabolic conditions
(e.g., hypercalcemia), malignancy, and infectious diseases
(13–15). Depressive symptoms that would otherwise be
diagnosable as major depressive disorder are diagnosed
instead as a mood disorder due to a general medical condition if the mood disturbance is judged to be the direct
physiological consequence of a specific general medical condition. Similarly, medications used to treat general medical
conditions may induce depressive syndromes. Such medications include transplant anti-rejection agents, chemotherapy agents, interferon, steroids, some antibiotics, and
others. Depression caused by medications is classified in
the DSM-IV-TR as other (or unknown) substanceinduced mood disorder (DSM-IV-TR code 292.84) (16).
Psychosocial stressors and other antecedent events,
and their possible contribution to the generation of depressive symptoms, should be explored in the course of a
psychiatric assessment. Depressive symptoms are a common response to psychosocial stressors, particularly bereavement. Symptoms characteristic of a major depressive
episode may arise after a significant loss; however, the diagnosis of major depressive disorder is generally not given
APA PRACTICE GUIDELINES
unless depressive symptoms are still present 2 months
after the loss, are particularly severe, or are uncharacteristic of or unrelated to bereavement, such as persistent
suicidal ideation or morbid preoccupation with worthlessness or guilt (16). Following a stressor, depressive symptoms that do not reach sufficient number or severity to be
classified as a major depressive episode may be better described as an adjustment disorder. Despite the possible
presence of antecedent stressors, psychiatrists should not
dismiss potentially disabling depressive symptoms as “normal,” thereby depriving patients of needed therapeutic attention.
A thorough assessment of depression also includes the
evaluation of psychotic symptoms. Major depressive disorder may be associated with mood-congruent and moodincongruent hallucinations and delusions. Depressed patients may not initially present with psychotic symptoms,
and patients may wish to hide shaming or distressing
thoughts. Therefore, psychiatrists should carefully query
patients about such symptoms in order to provide appropriate treatments for them (see Section III.A.2.a). Identifying the presence of atypical, melancholic, or catatonic
features of depression is also important, as such features
may influence the choice of treatments (see Sections
III.A.2.b, III.A.2.c, and III.A.2.d). Considering that major
depressive episodes are common in the course of bipolar I
disorder and that recurrent major depressive episodes are
characteristic of bipolar II disorder (17), it is important to
consider bipolar disorders as part of the differential diagnosis of major depressive disorder. This distinction is especially
important because the treatments for bipolar disorders often differ from those for major depressive disorder.
All patients who present for treatment for a major depressive episode should be screened for a past history of
manic or hypomanic episodes and for past adverse reactions to antidepressants that might be consistent with a
“switch” into hypomania or mania. Screening instruments
for manic and hypomanic episodes include the Mood Disorders Questionnaire (18) and the Screening Assessment
of Depression–Polarity, which includes three easily administered dichotomous questions (19). However, since
patients are often unaware of prior hypomanic or manic
episodes, even when questioned carefully, collateral
sources of information, such as family members living
with the patient, may be crucial in uncovering such episodes. Clinical assessment should also include whether or
not the patient is experiencing a mixed episode, which is
characterized by symptoms of both a major depressive episode and a manic episode that occur nearly every day for
at least 1 week.
It is also important to consider the frequency and chronicity of prior episodes of major depressive disorder.
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
Chronic forms of depression—such as dysthymic disorder,
“double depression” (dysthymic disorder and major depressive disorder), and major depressive disorder with the
“chronic” specifier—are all depressions with a duration of
at least 2 years. In clinical studies, chronic depression has a
lower response rate than nonchronic depression, but because the placebo-response rate is also lower, the relative
clinical benefit is comparable. The onset of benefit in
chronic depression appears more gradual than in nonchronic depression. However, despite a smaller response rate
and slower response, it is important to recognize that
chronic depression is not treatment refractory (20). Unfortunately, however, in many patients, chronic depression
remains undiagnosed or, if diagnosed, undertreated (21).
The presence of a family history of a mood disorder
should also be determined. Family histories of major depressive disorder and bipolar disorder are common in
those with major depressive disorder, but a family history
of bipolar disorder may indicate increased risk of bipolar
disorder in the patient. A family history of suicide is relevant in determining a patient’s suicide risk (22) and may
also signal the presence of an unrecognized mood disorder in a relative.
3. Evaluate the safety of the patient
Addressing safety concerns may take precedence over establishing a full differential diagnosis or completing the
psychiatric assessment. Because of the increased rates of
suicide in depressed patients (22–24), a thorough and ongoing evaluation of the patient’s suicide risk is essential.
Some components of an evaluation for suicidal risk are
summarized in Table 1. The psychiatrist should evaluate
the presence of suicidal ideation and behaviors, the extent
to which the patient has made plans for or begun to prepare
for suicide, the availability and lethality of the means for
suicide, and the degree to which the patient intends to act
on suicidal plans. A complete assessment also includes clinical factors that may increase the likelihood of a patient’s
acting on suicidal ideation, including a history of prior suicide attempts and the presence of psychotic symptoms, severe anxiety, panic attacks, impulsivity, and substance use.
Patients should also be asked about a family history of suicide and recent exposure to suicide or suicide attempts by
others. A suicide risk assessment should be individualized
to the particular circumstances of the patient by including
an evaluation of the patient’s strengths, motivation to seek
help, social support systems, and physical health.
Despite the best efforts of the psychiatrist, some patients may engage in self-harm (22). Even with careful assessments of suicide risk, the ability to predict suicidal
behavior is poor, with many false positives (i.e., patients
who appear more likely to make attempts or die by suicide
TABLE 1.
25
Factors to Consider in Assessing Suicide Risk
Lifetime history, nature, seriousness, and number of
previous attempts and aborted attempts
Presence, history, and lethality of suicidal ideation,
intent, or plans
Access to means for suicide and the lethality of those
means, such as access to a firearm
Presence of hopelessness, psychic pain, decreased
self-esteem, narcissistic vulnerability
Presence of severe anxiety, panic attacks, agitation,
impulsivity
Presence and history of aggression and violence
Nature of cognition, such as loss of executive function,
thought constriction (tunnel vision), polarized
thinking, closed-mindedness, poor coping and
problem-solving skills
Presence of psychotic symptoms, such as command
hallucinations or poor reality testing
Presence of alcohol or other substance use
Presence of major psychiatric disorders, such as major
depressive disorder, bipolar disorder, schizophrenia,
anorexia nervosa, alcohol use disorder, other substance
use disorders, cluster B personality disorders
Recent psychiatric hospitalization
Presence of disabling medical illness, especially with
poor prognosis, such as chronic pain, brain and spinal
cord injury, malignant neoplasm, HIV or acquired
immunodeficiency syndrome (AIDS), Huntington’s
disease, chronic hemodialysis-treated renal failure,
chronic obstructive pulmonary disease
Demographic features, such as age, race, marital status,
sexual orientation
Presence of acute or chronic psychosocial stressors, which
may include actual or perceived interpersonal losses,
financial difficulties or changes in socioeconomic status,
family discord, domestic partner violence, and past or
current sexual or physical abuse or neglect
Absence of psychosocial support, such as poor
relationships with family, unemployment, living alone,
unstable or poor therapeutic relationship, recent loss
of a relationship
History of childhood traumas, particularly sexual and
physical abuse
Family history of or recent exposure to suicide
Absence of protective factors, such as children in the
home, sense of responsibility to family, pregnancy,
life satisfaction, cultural beliefs, or religiosity
Source: Adapted from APA’s Practice Guideline for the Assessment
and Treatment of Patients With Suicidal Behaviors (22).
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26
but who do not) as well as false negatives (i.e., patients
who appear less likely to make attempts or die by suicide
but who do). The assessment of suicide risk is complicated
by the fact that suicidal individuals often conceal their
thoughts and plans or act impulsively on short-lived suicidal thoughts, making their response to direct questions
an unreliable predictor of dangerousness to self. For this
reason, in addition to using direct questioning, the psychiatrist should also obtain information through observation
and collateral history whenever possible (22, 25).
The risk of suicide should also be monitored as treatment proceeds, since variations in depressive symptoms
may be associated with fluctuations in suicide risk. In
youth and young adults, increases in suicidal thoughts and
attempts have been reported early in the course of treatment with antidepressants, although no increases in mortality rates were seen in clinical trials (26). Family members
can provide information that increases the likelihood of
early detection of harmful behaviors. It is also useful to
convey the expectation that family members will call the
psychiatrist if concerns for safety emerge (27). For information about how suicidal ideation or behaviors affect the treatment plan, see Section III.A.1.a.
Although the greatest risk surrounding depression involves the patient’s health, a rare but also potentially disastrous outcome of depression is violence toward others,
including homicide (28, 29). Psychosis, substance abuse,
impulsivity, and a history of aggression increase this risk
(30–32). Psychiatrists accordingly should assess not only
suicidal risk but also history of violence, homicidal ideation, and plans of violence toward others. Additional assessment may be necessary under specific circumstances.
For example, it is important to assess the impact of parental depression (including peripartum depression) on
children in the home, with specific attention given to the
parent’s vulnerability to neglect or harm the children (33).
Whenever suicidal or violent ideas are expressed or suspected, careful documentation of the decision-making process is essential. In addition, patients who exhibit suicidal
or violent ideas or intent require close monitoring.
4. Establish the appropriate setting for treatment
Treatment settings for patients with major depressive disorder include a continuum of possible levels of care, from
involuntary hospitalizations to partial hospital programs,
skilled nursing homes, and in-home care. In general, patients should be treated in the least restrictive setting that
is most likely to prove safe and effective. The psychiatrist
should choose an appropriate site of treatment after evaluating the patient’s clinical condition, including symptom
severity, co-occurring conditions, level of functioning, and
available support system. The estimated degree of risk to
APA PRACTICE GUIDELINES
self and to others is another significant determinant of
treatment setting. Decisions about treatment setting
should also include consideration of the patient’s ability to
adequately care for him- or herself, provide reliable feedback to the psychiatrist, and cooperate with treatment of
the major depressive disorder.
Patients with suicidal or homicidal ideation, intention,
or plans require close monitoring. For those at significant
risk, measures such as hospitalization should be considered; hospitalization is usually indicated for patients who
are considered to pose a serious threat of harm to themselves or others. Patients who refuse can be hospitalized
involuntarily if their condition meets the criteria of the local jurisdiction for involuntary admission. Severely ill patients who lack or reject adequate social support outside of
a hospital setting should be considered for admission to a
hospital or intensive day program, if available. In addition,
patients who also have complicating psychiatric or general
medical conditions or who have not responded adequately
to outpatient treatment may need to be hospitalized.
The optimal treatment setting and the patient’s likelihood of benefit from a different level of care should be
reevaluated on an ongoing basis throughout the course of
treatment. Unfortunately, the spectrum of treatment settings available to patients is often limited by lack of availability of options in the geographic setting, lack of ability
to pay for care, and/or limitations imposed by third party
payers.
5. Evaluate functional impairment and quality of life
The assessment of a patient with major depressive disorder
includes a determination of the severity and chronicity of
symptoms. Even mild depression can impair function and
threaten life and the quality of life. In the extreme, depressed people may be totally unable to function socially
or occupationally or even to feed and clothe themselves
and maintain minimal personal hygiene. Severely depressed
patients may be immobilized to the point of being bedridden, with associated medical complications.
The psychiatrist should address impairments in functioning and help the patient to set specific goals appropriate
to his or her functional impairments and symptom severity.
This will likely involve helping the patient to establish intermediate, pragmatic steps in the course of recovery. For
example, the psychiatrist may help patients who are having
difficulty meeting commitments to develop a reasonable
plan to fulfill their obligations (e.g., work, family obligations), potentially by making alternative arrangements.
The psychiatrist may advise other patients not to make major life changes while in the midst of a major depressive
episode. Impairments in the patient’s overall quality of life
should also be assessed, which can be done by asking pa-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
tients what bothers them the most about their depression
and determining how their current activities and enjoyment of life have been altered by their depressive symptoms. The overall goals of treatment of major depressive
disorder should focus on alleviating functional impairments and improving quality of life in addition to achieving
symptom resolution and episode remission.
6. Coordinate the patient’s care with other clinicians
The psychiatrist should assure that a comprehensive assessment of general medical conditions is performed in order
to identify factors that may precipitate or exacerbate depressive symptoms. He or she may initiate the medical
evaluations or coordinate care with other appropriate clinicians. In some situations, review of medical records provided
by the patient will suffice. In other situations, particularly
when medical treatment is indicated, the psychiatrist should,
with the patient’s permission, arrange for collaborative care
with other clinicians. Such collaboration may incorporate
discussion of prescribed medication, including dose changes
and possible drug interactions as well as necessary diagnostic procedures and medical monitoring, which may include
laboratory measures and ECG (34).
In treating the patient’s depressive illness, a multifaceted
approach is typically required that may include provision
of depression-focused psychotherapy, pharmacotherapy,
ECT, or other therapeutic approaches. Under some circumstances, all aspects of treatment will be administered
by one psychiatrist, and this model of care may improve
integration of treatment components (35) or reduce overall treatment cost (36). In other situations, treatment may
require the coordinated effort of several clinicians. This
decision is frequently influenced by the clinicians’ expertise in providing the indicated therapeutic modality,
economic factors, availability of treatment, and by the patient’s preferences. When this treatment model is used,
one team member must assume the primary overall responsibility for the patient’s care. This individual serves as
the coordinator of the treatment plan, advocates for the
appropriate level of care, oversees the family involvement,
makes decisions regarding which potential treatment modalities are useful and which should be discontinued, helps
assess the effects of medications, and monitors the patient’s safety. Because of the diversity and depth of medical
knowledge and expertise required for this oversight function, a psychiatrist is generally optimal for this role, although this staffing pattern may not be possible in some
health care settings. If the treatment is split, the psychiatrist who is providing the psychiatric management and the
medication treatment should meet with the patient frequently enough to monitor his or her care. Ongoing co-
27
ordination of the overall treatment plan is essential and is
enhanced by clear role definitions, plans for the management of crises or relapses, and regular communication
among the clinicians who are involved in the treatment.
Psychiatrists may at times serve as consultants to ongoing treatment of depression by other prescribers. Health
care professionals other than psychiatrists may prescribe
antidepressant medication for their patients for a variety of
reasons, including convenience, financial reasons, stigma,
and access to care issues (37). Primary care doctors, obstetricians, and physicians of other disciplines may screen for
depression and initiate treatment for patients. In fact, at
least one-fourth of patients presenting to primary care settings may have major depressive disorder, and 70%–80%
of antidepressants are prescribed by a primary care physician
or medical subspecialist (38, 39). Regardless of whether the
psychiatrist is acting as a consultant or transferring ongoing care to another clinician (e.g., with transition from an
inpatient to outpatient setting), communication and coordination of treatment are essential. Optimal communication with other health care professionals can improve
overall treatment by assuring that medical conditions and
psychosocial issues are appropriately addressed. Good communication also decreases the risk that patients will receive
inconsistent information about treatment options and risks
and benefits. Furthermore, communication among clinicians improves vigilance against relapse, side effects, and risk
to self or others.
7. Monitor the patient’s psychiatric status
As treatment progresses, different features and symptoms
of the patient’s illness may emerge or subside. The psychiatrist should carefully and systematically monitor changes
in the patient’s psychiatric status, including major depressive disorder symptoms, as well as symptoms of other potential co-occurring conditions (Table 2). Monitoring the
patient’s status for the emergence of or changes in destructive impulses toward self or others is especially crucial; additional measures such as hospitalization or more intensive
treatment should be considered for patients found to be at
higher risk. In addition, the patient should be monitored
for treatment-emergent side effects, some of which may be
difficult to distinguish from symptoms of the underlying
depressive disorder or co-occurring medical conditions.
Significant changes in a patient’s psychiatric status or the
emergence of new symptoms may warrant a diagnostic reevaluation of the patient. For example, patients who note
worsening irritability, increased difficulty sleeping, racing
thoughts, growing impulsivity, euphoria, or rapid shifts in
mood should be monitored more closely and may warrant
re-evaluation and consideration of a possible bipolar dis-
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28
order diagnosis. Often family members or caregivers notice
changes in the status of the patient first and are therefore
able to provide valuable input to the psychiatrist.
8. Integrate measurements into psychiatric management
The integration of measurement tools into psychiatric management, which has been referred to as measurement-based
care, may enhance the quality of care and improve clinical
outcomes (40). Clinician-rated and/or self-rated scales can
help determine the trajectory of disease course and effects
of treatment. Many such scales are available in several versions that vary by number of items. Self-rated scales are convenient to use but require review, interpretation, and discussion with the patient. In research studies, commonly used
tools include the Inventory of Depressive Symptoms (IDS),
which is available in clinician-rated and self-rated versions
(http://www.ids-qids.org/), the clinician-rated Hamilton
Rating Scale for Depression (HAM-D) (http://healthnet.
umassmed.edu/mhealth/HAMD.pdf) (41, 42), the clinicianrated Montgomery Asberg Depression Rating Scale
(MADRS) (http://www.cnsforum.com/streamfile.aspx?file
name=MADRS.pdfandpath=pdf) (43), and the self-rated 9item Patient Health Questionnaire (PHQ-9) (http://www.
depression-primarycare.org/clinicians/toolkits/materials/
forms/phq9/) (44, 45). The Beck Depression Inventory
(BDI, BDI-II) is another commonly used, copyrighted, 21question multiple-choice self-rated instrument (46).
Systematic measurement of side effects can also assist in
the provision of treatment. Several self-report rating scales
have been developed for assessing side effects of antidepressant treatment and are available in English and Spanish versions (http://www.edc.pitt.edu/stard/public/ assessment_
forms.html). The Frequency, Intensity, and Burden of Side
Effects Rating Scale (FIBSER), which has also been referred to as the Frequency and Intensity of Side Effects
Rating/Global Rating of Side Effect Burden, uses three
global Likert scale ratings to assess side effects experienced
over the preceding week (47, 48). The Patient Rated Inventory of Side Effects (PRISE) is a 9-item scale that asks patients about the presence of side effects in eight organ system
domains, as well as about other side effects (47, 48). A clinician-administered scale, the Toronto Side Effects Scale,
that focuses on antidepressant medication side effects is
also available (http://ww1.cpa-apc.org:8080/publications/
archives/cjp/2002/march/orAntidepressantsAppendix.asp)
(49). The Udvalg for Kliniske Undersøgelser (UKU) side
effect rating scale (50) (available at http:/ /www.cnsforum.
com/streamfile.aspx?filename=UKU. pdfandpath=pdf) is
often used in research studies and may offer clinicians additional questions that could be asked about side effects,
but it is likely to be too detailed for routine clinical use.
APA PRACTICE GUIDELINES
TABLE 2.
Items to Monitor Throughout Treatment
Symptomatic status, including functional status, and
quality of life
Degree of danger to self and others
Signs of “switch” to mania
Other mental disorders, including alcohol and other
substance use disorders
General medical conditions
Response to treatment
Side effects of treatment
Adherence to treatment plan
Although the use of rating scales is not yet common
practice in clinical settings, in part due to pragmatic concerns (51), the use of such scales can be valuable in monitoring symptoms and treatment progress. In addition,
electronic monitoring is becoming more feasible, as electronic health records are more commonly utilized and
patients and psychiatrists have increased access to technological tools that can help monitor and record symptoms.
Baseline data and information about treatment-emergent
changes can be collected systematically from the patient
and electronically transmitted via telephone or the Internet. In addition to providing secure electronic capture of
patient data, computerized decision support systems can
be useful in implementing evidence-based treatment for
major depressive disorder (52).
9. Enhance treatment adherence
For treatment to be successful, it is essential to support the
patient’s adherence to all details of the regimen by providing education about the illness and its treatment, maintaining a strong therapeutic alliance, mobilizing family and
other supports (including eliciting questions and clarifying
common misconceptions), evaluating factors affecting adherence, and addressing barriers to adherence as they arise.
Major depressive disorder is often a chronic or recurrent
condition that requires patients to participate actively in
and adhere to treatment plans for long periods, despite the
fact that side effects or requirements of treatments may be
burdensome. Patients may have strong preferences for modality of treatment or medication choice, particularly if
they or a family member have had past experience with the
treatment or medication. When feasible, factoring in these
preferences may improve adherence to treatment. During
the acute phase, patients with major depressive disorder
may be poorly motivated, unduly pessimistic about their
chances of recovery with treatment, suffering from deficits
in memory, or poorly caring for themselves. During the
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
maintenance phase, euthymic patients may undervalue the
benefits of and focus on the burdens of treatment. The psychiatrist should recognize these possibilities, emphasize the
importance of adherence for successful treatment and prophylaxis, and encourage the patient to articulate any concerns regarding adherence (e.g., side effects, costs of treatment, scheduling conflicts, lack of transportation or child
care). Patient and family attitudes about depression and its
treatment can also influence adherence. Family members
can play an important role in promoting optimism about
treatment, assisting patients with adherence and providing
the psychiatrist with input on side effects or other treatment-related concerns that may influence adherence.
Some aspects of adherence will vary with the type of
treatment being used. For example, patients in psychotherapy may experience increased anxiety as they confront fearful or difficult topics. This anxiety, in turn, may decrease
adherence to psychotherapy, and patients may begin to arrive late to or miss therapy sessions. In patients who are
beginning treatment with a medication, common side effects of medication options should be discussed. Patients
should be involved in treatment decisions and encouraged
to convey input on side effects that they consider reasonable or unbearable. Side effects such as weight gain, cognitive dulling, sexual side effects, sedation or fatigue, and
agitation may represent different burdens to different individuals. Emphasizing the following specific topics improves adherence: 1) explaining when and how often to
take the medicine; 2) suggesting reminder systems, such
as pill boxes, alarms, etc.; 3) discussing the need to take
medication for at least 2–4 weeks before beneficial effects
may be noticed; 4) emphasizing the need to take medication even after feeling better; 5) reviewing the need to
consult with the psychiatrist before discontinuing medication; 6) giving the patient an opportunity to express his
or her understanding of the medication, hearing his or her
concerns, and correcting any misconceptions, and 7) explaining what to do if problems or questions arise (53).
Behavioral tailoring, which involves developing an individualized approach to incorporating medication into the
daily routine and can also include simplifying the medication regimen, has demonstrated efficacy for individuals
with schizophrenia and may also be applicable to individuals
with other psychiatric illnesses (54). Adherence may also
be improved by minimizing the cost and complexity of
medication regimens. Most antidepressant medications
are available in generic forms, which are generally less
costly. For individuals who cannot afford needed medications, some pharmaceutical companies offer patient assistance programs. Information on such programs is
available from pharmaceutical company Web sites, from
the Web site of the Partnership for Prescription Assistance
29
(http://www.helpingpatients.org), and from Rx Assist
(http://www.rxassist.org).
10. Provide education to the patient and the family
Education concerning major depressive disorder and its
treatments should be provided to all patients. Education is
an essential element of obtaining informed consent to
treatment. Whenever possible, education should also be
provided to involved family members and significant others, although generally the patient’s consent is required
before such information can be shared. Specific topics to
discuss may include that major depressive disorder is a
medical illness and that effective treatments are both necessary and available. This information may be especially
important for patients who attribute their illness to a
moral defect, or for family members who are convinced
that there is nothing wrong with the patient. Education
regarding available treatment options will help patients
make informed decisions, anticipate side effects, and adhere to treatments. Patients with depression can become
easily discouraged in treatment, especially if there is less
than a full initial response. The psychiatrist should encourage and educate patients to distinguish between the
hopelessness that is a symptom of depression and the relatively hopeful actual prognosis. In addition, for patients
treated with antidepressant medication or ECT, psychiatrists may choose to discuss a predictable progression of
treatment effects: first, side effects may emerge, then neurovegetative symptoms remit, and finally mood improves.
Often significant others notice symptomatic improvement before the patient does.
Given the chronic, episodic nature of major depressive
disorder, exacerbations are common. Patients, as well as
their families, if appropriate, should be instructed about
the significant risk of relapse. They should be educated
to identify early signs and symptoms of new episodes and
the stressors that may precede them. Patients should also
be instructed to seek adequate treatment as early in the
course of the new episode as possible to decrease the likelihood of a full-blown exacerbation or complications.
Patient and family education also includes general promotion of healthy behaviors such as good sleep hygiene
and decreased use of caffeine, tobacco, alcohol, and other
potentially deleterious substances. For most individuals,
exercise carries benefits for overall health. Data generally
support at least a modest improvement in mood symptoms for patients with major depressive disorder who engage in aerobic exercise (55–61) or resistance training
(62, 63). Regular exercise may also reduce the prevalence
of depressive symptoms in the general population, with
specific benefit found in older adults (64, 65) and individuals with co-occurring medical problems (57, 66).
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30
B. ACUTE PHASE
1. Choice of initial treatment modality
The acute phase of treatment lasts a minimum of 6–12
weeks. During this phase, the aims of treatment are to induce remission of symptoms and achieve a full return to
the patient’s baseline level of functioning. In addition to
general psychiatric management (described in Section
II.A), treatment may consist of pharmacotherapy or other
somatic therapies (e.g., ECT, light therapy), depressionfocused psychotherapy, or the combination of somatic and
psychosocial therapies. Selection of an initial treatment modality is influenced by several factors, including the symptom profile, the presence of co-occurring disorders or
psychosocial stressors, the patient’s prior treatment experience, and the patient’s preference.
Psychiatrists should present patients with information
concerning the evidence for a broad range of treatment
options, including somatic therapies and psychosocial interventions. Antidepressant medications can be used as an
initial treatment modality by patients with mild, moderate, or severe major depressive disorder. Clinical features
that may suggest that medications are the preferred treatment modality include a history of prior positive response
to antidepressant medications, the presence of moderate
to severe symptoms, significant sleep or appetite disturbances, agitation, patient preference, and anticipation of
the need for maintenance therapy. Patients with major depressive disorder with psychotic features require either
the combined use of antidepressant and antipsychotic
medications or ECT.
Psychotherapy may also be considered as monotherapy
for patients with mild to moderate major depressive disorder. The availability of clinicians with appropriate training and expertise in specific psychotherapeutic approaches
can be a factor in choosing a psychotherapy (67). Other
factors that can influence this choice may be the psychosocial context, patient preference, prior positive response
to psychotherapy, the presence of significant psychosocial
stressors or interpersonal difficulties, co-occurring Axis II
disorders, or the stage, chronicity, and severity of the major
depressive episode. Specifically, many severely depressed
patients will require both a depression-focused psychotherapy and a somatic treatment such as pharmacotherapy.
Pregnancy, lactation, or the wish to become pregnant may
tilt a decision toward psychotherapy as an initial treatment
(see Section III.B.6). Given the lower occurrence of side effects and suggestion of enduring benefits associated with
depression-focused psychotherapies (68), such treatments
might be preferable alternatives to pharmacotherapy for
some patients with mild to moderate depression.
APA PRACTICE GUIDELINES
Combining a depression-focused psychotherapy and
pharmacotherapy may be a useful initial treatment choice
for patients with moderate to severe major depressive disorder. Other indications for combined treatment include
chronic forms of depression, psychosocial issues, intrapsychic conflict, interpersonal problems, or a co-occurring Axis II disorder. In addition, patients who have had a
history of only partial response to adequate trials of single
treatment modalities may benefit from combined treatment. Poor adherence with pharmacotherapy may also
warrant combined treatment with medications and psychotherapy focused on treatment adherence.
Electroconvulsive therapy should be considered as a potential treatment option for all patients with major depressive disorder who have psychotic features or catatonia and
for those with an urgent need for response, such as patients
who are suicidal or who are nutritionally compromised as a
result of refusing food. Electroconvulsive therapy may also
be the treatment modality of choice for patients with major
depressive disorder who have a high degree of symptom
severity. Other considerations include the presence of cooccurring general medical conditions that preclude the use
of antidepressant medications, a prior history of positive response to ECT, and patient preference. Evidence for TMS
is currently insufficient to support its use in the initial treatment of major depressive disorder.
If a patient with mild depression wishes to try exercise
alone for several weeks as a first intervention, there is little to
argue against it (Section II.A.10), provided the patient is sufficiently monitored for an abrupt worsening of mood or adverse physical effects (e.g., ischemia or musculoskeletal
symptoms). The dose of exercise and adherence to an exercise regimen may be particularly important to monitor in the
assessment of whether an exercise intervention is useful for
major depressive disorder (69, 70). If mood fails to improve
after a few weeks with exercise alone, the psychiatrist should
recommend medication or psychotherapy. For patients with
depression of any severity and no medical contraindication
to exercise, physical activity is a reasonable addition to a
treatment plan for major depressive disorder. The optimal
regimen is one the patient prefers and will adhere to.
Figure 1 summarizes treatment modalities that may be
appropriate during the acute phase of treatment depending on the severity of the patient’s symptoms and other associated features of the depressive episode. It is important
to note that other factors may be relevant to treatment decisions for individual patients and that determinations of
episode severity are imprecise, although rating scales may
be helpful in assessing the magnitude of depressive symptoms and their effects on functional status and quality of
life (see Sections II.A.7 and II.A.8).
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31
Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
Modality
Pharmacotherapy in
Combination With
Depression-Focused
Psychotherapy
Electroconvulsive
Therapy
Pharmacotherapy
Depression-Focused
Psychotherapy
Mild to Moderate
Yes
Yes
May be useful for
patients with psychosocial or interpersonal
problems, intrapsychic conflict, or
co-occurring Axis II
disorder
Yes, for certain
patients
Severe Without
Psychotic Features
Yes
No
Yes
Yes
Severe With
Psychotic Features
Yes, provide both
antidepressant and
antipsychotic
medication
No
Severity of Illness
FIGURE 1.
Yes, provide both
antidepressant and
antipsychotic
medication
Yes
Recommended Modalities for Acute Phase Treatment of Major Depressive Disorder
2. Pharmacotherapy
Antidepressant medications have been grouped as follows:
1) TCAs, which for the purposes of this guideline also
include the tetracyclic antidepressant medication maprotiline; 2) SSRIs, which include fluoxetine, sertraline,
paroxetine, fluvoxamine, citalopram, and escitalopram;
3) SNRIs, which include venlafaxine, desvenlafaxine, and
duloxetine; 4) other antidepressant medications, including bupropion, nefazodone, trazodone, and mirtazapine;
and 5) MAOIs, which include phenelzine, tranylcypromine, isocarboxazid, and the transdermal formulation of
selegiline. Although some studies have suggested superiority of one mechanism of action over another, there are
no replicable or robust findings to establish a clinically
meaningful difference. For most patients, the effectiveness of antidepressant medications is generally comparable
between classes and within classes of medications. Response
rates in clinical trials typically range from 50% to 75% of
patients, with some evidence suggesting greater efficacy
relative to placebo in individuals with severe depressive
symptoms as compared with those with mild to moderate
symptoms (71–73). Although remission rates are less robust
and selective publication of positive studies could affect the
apparent effectiveness of treatment (74, 75), these factors
do not appear specific to particular medications or medication classes.
Nevertheless, antidepressant medications do differ in
their potential to cause particular side effects such as adverse
sexual effects, sedation, or weight gain. Therefore, the
initial selection of an antidepressant medication will
largely be based on the tolerability, safety, and cost of the
medication, as well as patient preference and history of
prior medication treatment (Table 3). Other factors include the medication half-life and potential for drug interactions related to properties such as plasma protein
binding or metabolism through the cytochrome P450
system (Tables 4 and 5). On the basis of these considerations, the following medications are optimal for most
patients: SSRIs, SNRIs, mirtazapine, and bupropion.
Table 6 provides the starting and usual doses of medications that have been shown to be effective for treating
major depressive disorder.
TABLE 3.
Factors to Consider in Choosing an Antidepressant
Medication
Patient preference
Nature of prior response to medication
Relative efficacy and effectiveness
Safety, tolerability, and anticipated side effects
Co-occurring psychiatric or general medical
conditions
Potential drug interactions
Half-life
Cost
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32
TABLE 4.
APA PRACTICE GUIDELINES
Cytochrome P450 Enzyme Metabolism of Antidepressive Agents
a
1A2
2B6
2C9
2C19
2D6
3A4
Amitriptyline
+
+
++
++
++
+
Bupropion
b
Hydroxybupropion
+
++
+
Citalopram
Desipramine
+
++
++
+
+
++
Desvenlafaxine
Duloxetine
+
++
++
Escitalopram
Fluoxetine
b
Norfluoxetine
+
+
Imipramine
++
+
Maprotiline
+
Mirtazapine
b
8-Hydroxymirtazapine
b
Mirtazapine-N-oxide
++
Nortriptyline
+
++
++
+
+
+
++
+++
+
++
++
++
++
+
+
++
++
+
++
++
++
+
Paroxetine
++
Protriptyline
++
Selegiline
Sertraline
++
+
++
++
Venlafaxine
b
O-Norvenlafaxine
+
+
+
++
+
+
+
+
++
++
+
Sources: (82, 83). The extent to which each medication is a substrate for a specific enzyme is indicated as follows: +++ = exclusive substrate, ++ = major substrate, + = minor substrate.
a
Information about drug metabolism and drug-drug interactions is constantly evolving. The information in this table can serve as a
guide; however, the reader is encouraged to access regularly updated online sources of drug-drug interactions.
b
Active metabolite of parent compound.
In choosing an antidepressant medication, many psychiatrists also consider the family history of response to
particular medications; however, the impact of this factor
on the likelihood of the patient’s response to these medications is unclear. Nevertheless, the medication experiences
of others close to the patient do influence the patient’s belief about particular medications and pharmacotherapy in
general.
The presence of co-occurring psychiatric or general
medical conditions can be a significant factor influencing
the choice of an antidepressant medication. For example,
TCAs are generally not optimal in patients with cardiovascular conditions, cardiac conduction defects, closed angle
glaucoma, urinary retention, significant prostatic hypertrophy, or eating disorders with significant malnutrition
or purging. In older adults and others with malnutrition,
autonomic disorders (e.g., diabetic neuropathy, Parkinson’s disease), or low blood pressure, TCAs may exacerbate hypotension and orthostasis, resulting in syncope or
falls. Selective serotonin reuptake inhibitors and SNRIs
may be inappropriate for patients who are experiencing
sexual dysfunction. Patients who are receiving tamoxifen
for breast cancer or other indications should generally be
treated with an antidepressant (e.g., citalopram, escitalopram, venlafaxine, desvenlafaxine) that has minimal effect
on metabolism through the cytochrome P450 2D6 isoenzyme, because reduced metabolism of tamoxifen through
CYP 2D6 is likely to be associated with lower levels of
tamoxifen’s active metabolite (76–79) with the possibility of
poorer patient outcomes (80, 81).
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33
Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
Cytochrome P450 Enzyme Inhibition by Antidepressive Agents
TABLE 5.
1A2
Amitriptyline
2A6
2B6
a
2C8
+
2C9
2C19
2D6
+
2E1
3A4
+
Bupropion
+++
Citalopram
+
b
+
++
Desipramine
+
++
+
++
+
Desvenlafaxine
+
Duloxetine
++
Escitalopram
++
Fluoxetine
c
Norfluoxetine
Imipramine
++
+
+
Mirtazapine
+
Nortriptyline
++
++
++
++
+
+
++
+
++
+
Selegiline
+
Sertraline
Desmethylsertralinec
Venlafaxine
+
+
+
+
+
d
Paroxetine
+++
++
+
+++
+
++
+
+
+
+
+
+
+++
+
+
+
+
+
++
++
+
+
+
++
+
+
+
++
+
+
Sources: (82, 83). The extent to which each medication is a substrate for a specific enzyme is indicated as follows: +++ = strong inhibitor, ++ = moderate inhibitor, + = weak inhibitor.
a
Information about drug metabolism and drug-drug interactions is constantly evolving. The information in this table can serve as a
guide; however, the reader is encouraged to access regularly updated online sources of drug-drug interactions.
b
c
d
Also a metabolite of imipramine. Active metabolite of parent compound. Also a metabolite of amitriptyline.
Because of the need for dietary restrictions and the potential for serious side effects and drug interactions, use of
MAOIs is generally limited to patients who do not respond to other treatments. MAOIs may be particularly
effective for patients with major depressive disorder with
atypical features, although many psychiatrists prefer to
prescribe SSRIs for such patients because of SSRIs’ greater
safety and tolerability and more favorable adverse effect
profile.
a.
Efficacy of antidepressant medications
1. Selective serotonin reuptake inhibitors
Selective serotonin reuptake inhibitors currently available
include fluoxetine, sertraline, paroxetine, fluvoxamine,
citalopram, and escitalopram. A large body of literature
supports the superiority of SSRIs compared with placebo
in the treatment of major depressive disorder. In more
than 10 systematic reviews and meta-analyses, the effectiveness of SSRIs has been compared with that of other antidepressant medications, mainly TCAs. The SSRIs have
demonstrated comparable efficacy to the TCAs (84–88),
even when anxiety symptoms are considered (85, 87–90).
Although a few analyses suggest small advantages of
SNRIs over SSRIs in rates of remission (91), a preponderance of the data finds no significant evidence of the superiority of any other class or agents over SSRIs (84, 89, 90,
92–95). One meta-analysis suggests a slight superiority of
escitalopram compared with other SSRIs and venlafaxine
(93), and another found significantly greater efficacy for
escitalopram, sertraline, venlafaxine, and mirtazapine as
compared with duloxetine, fluoxetine, fluvoxamine, and
paroxetine (96), but other studies show no differences in
efficacy among individual SSRIs (84, 93–95, 97, 98).
2. Serotonin norepinephrine reuptake inhibitors
The serotonin norepinephrine reuptake inhibitors currently
available are venlafaxine, desvenlafaxine (the principal
metabolite of venlafaxine), and duloxetine. An immediaterelease form of venlafaxine is available, but most clinicians
prefer the extended-release formulation because it is approved for once-daily dosing and may be less often associated with reported withdrawal symptoms.
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34
TABLE 6.
APA PRACTICE GUIDELINES
Dosing of Medications Shown To Be Effective in Treating Major Depressive Disorder
a
Starting Dose
b
(mg/day)
Generic Name
Usual Dose
c
(mg/day)
Selective serotonin reuptake inhibitorsd
Citalopram
Escitalopram
Fluoxetine
20
10
20
20–60e
10–20
e
20–60
Paroxetine
Paroxetine, extended release
Sertraline
20
12.5
50
20–60
25–75
e
50–200
e
d
Dopamine norepinephrine reuptake inhibitor
Bupropion, immediate release
Bupropion, sustained release
Bupropion, extended release
Serotonin norepinephrine reuptake inhibitorsd
Venlafaxine, immediate release
Venlafaxine, extended release
Desvenlafaxine
Duloxetine
Serotonin modulators
Nefazodone
Trazodoneg
Norepinephrine-serotonin modulator
d
Mirtazapine
Tricyclics and tetracyclics
Amitriptyline
Doxepin
Imipramine
Desipramine
Nortriptyline
Trimipramine
Protriptyline
Maprotiline
Monoamine oxidase inhibitors (MAOIs)
Irreversible, nonselective inhibitors
Phenelzine
Tranylcypromine
Isocarboxazid
Irreversible, MAO B selective inhibitor
h
Selegiline transdermal
Reversible MAO A selective inhibitor
Moclobemide
150
150
150
37.5
37.5
50
60
300–450
300–400
300–450
75–375
75–375
f
50
60–120
50
150
150–300
150–600
15
15–45
25–50
25–50
25–50
25–50
25
25–50
10–20
75
100–300
100–300
100–300
100–300
50–200
75–300
20–60
100–225
15
10
10–20
45–90
30–60
30–60
6
6–12
150
300–600
a
For convenience, medications other than TCAs have been classified by their presumptive mechanism of action. However, the exact
b
mechanism of action of several medications has yet to be determined or varies by dose. Lower starting doses are recommended for
elderly patients and for patients with panic disorder, significant anxiety or hepatic disease, and co-occurring general medical conditions.
c
For some of these medications (e.g., TCAs) the upper dosing limit reflects risk of toxicity or need for plasma level assessment, whereas
d
for other medications (e.g., SSRIs), higher doses can be used safely but without evidence for overall superior efficacy. These medications are likely to be optimal medications in terms of safety, the patient’s acceptance of side effects, and the quantity and quality of clinical
e
f
trial data. Dose varies with diagnosis; see text for specific guidelines. Has been used at doses up to 400 mg/day, although doses above
g
h
50 mg/day may not provide additional benefit. This medication is not typically used for this indication. Selegiline selectively inhibits
MAO B at low doses but inhibits both MAO A and MAO B at the higher doses that are typically required for antidepressant activity.
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
Each of these medications is efficacious (i.e., superior
to placebo in controlled studies and meta-analyses) (95,
99), and venlafaxine (75–150 mg/day) and duloxetine
(60 mg/day) showed comparable efficacy in a pair of trials
(100). For venlafaxine and perhaps desvenlafaxine, clinically significant norepinephrine reuptake inhibition may
not be achieved for the average patient at lower therapeutic doses, although desvenlafaxine has a much greater
bioavailability, resulting in a lower effective dose. In individual studies, venlafaxine and duloxetine are generally as
effective as SSRIs (see the meta-analyses of Nemeroff et
al. [101] and Thase et al. [102] for tabulated summaries of
individual study results from the more than 40 relevant
randomized controlled trials). Results of comparative
studies of desvenlafaxine are not known at this time. Relative to SSRIs, some analyses of pooled data sets have suggested a small advantage for SNRIs (91), which might
afford clinically modest benefits for patients with more severe depression (102) or for patients who have not responded to prior trials of SSRIs (103). However, other
meta-analyses have shown equivalent efficacy for SSRIs
and SNRIs (95), whereas some have shown superiority of
individual medications but no clearcut medication class
effects (96). Relative to TCAs, venlafaxine’s efficacy is
comparable (91, 104, 105), whereas the more recently introduced duloxetine and desvenlafaxine have not been
systematically compared with TCAs.
3. Other antidepressant medications
A number of other antidepressant medications differ structurally or in their pharmacological action from medications
in the categories just described and are included here.
Although bupropion is classified as a norepinephrine
and dopamine reuptake inhibitor, the latter effect is relatively weak, and its mechanism of action remains unclear
(106). There are three formulations of bupropion: immediate release, sustained release, and extended release.
Bupropion is distinct from most antidepressants in not
having an indication for the treatment of any primary
anxiety disorder, and it may be less well tolerated than
other antidepressants among patients with significant
anxiety. In addition, a meta-analysis showed that SSRIs
were modestly superior to bupropion for a subset of patients with major depressive disorder and anxiety (107).
For individuals with low to moderate levels of anxiety, the
same meta-analysis showed that the efficacy of bupropion
in treating major depressive disorder was roughly comparable to that of the SSRIs (107). Results of another
meta-analysis suggested that bupropion may be more likely
to improve symptoms of fatigue and sleepiness than at
least some of the SSRIs (108). Bupropion may be a good
choice for patients who have a goal of quitting smoking as
it has U.S. Food and Drug Administration (FDA) approval
35
for this indication, reduces desire for nicotine, and doubles rates of smoking cessation (109, 110). Patients typically experience minimal weight gain or even weight loss
on bupropion (111), and for this reason it may be an appropriate antidepressant for patients who are overweight
or obese.
Mirtazapine is thought to work through noradrenergic
and serotonergic mechanisms, although this tetracyclic
compound is not a reuptake inhibitor (112). Mirtazapine
has comparable efficacy to SSRIs (113).
Trazodone is the oldest medication from this group
that is still in wide use. Although trazodone is an effective
antidepressant, relative to placebo (105, 114, 115), in contemporary practice it is much more likely to be used in
lower doses as a sedative-hypnotic than as an antidepressant. Despite widespread use of trazodone as a hypnotic,
few data support its use for this indication.
Nefazodone has an analogous structure to trazodone but
somewhat different pharmacological properties. In comparative trials versus SSRIs, nefazodone showed comparable efficacy and overall tolerability (116).
4. Tricyclic antidepressants
Tricyclic antidepressants (amitriptyline, nortriptyline,
protriptyline, imipramine, desipramine, doxepin, and trimipramine) are effective treatments for major depressive
disorder and have comparable efficacy to other classes of
antidepressants, including SSRIs, SNRIs, and MAOIs
(85, 105). The efficacy of subclasses of tricyclics (e.g., secondary amines or tertiary amines) appears to be comparable. TCAs may be particularly effective in certain
populations, such as in hospitalized patients (117, 118).
Conventional wisdom is that this advantage is explained
by the superiority of TCAs (versus SSRIs) among the subset
of patients with melancholia or more severe depression,
because such a specific advantage has not been consistently documented in studies of less severely ill outpatients (85, 105, 118).
5. Monoamine oxidase inhibitors
MAOIs currently used as antidepressants include phenelzine, tranylcypromine, isocarboxazid, moclobemide, and
the transdermally delivered formulation of selegiline.
MAOIs have comparable efficacy to other antidepressants for outpatients with major depressive disorder and
may be appropriate for patients with major depressive disorder who have not responded to safer and more easily
used treatments (119, 120). In fact, the role of MAOIs in
major depressive disorder is now almost exclusively reserved for patients who have not responded to at least several other pharmacotherapies. Studies have demonstrated
the effectiveness of MAOIs in patients who have not responded to other antidepressant medications, particularly
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36
TCAs (119). However, the effectiveness of MAOIs relative to other strategies for treatment-resistant patients in
contemporary practice remains unclear, particularly for
patients who have not responded to multiple sequential
trials with SSRIs and SNRIs (121).
MAOIs have been shown to be particularly effective in
treating depressed patients with atypical features, so psychiatrists should consider using these medications for patients with symptoms such as reactive moods, reverse neurovegetative symptoms, and sensitivity to rejection (119,
120, 122). There do not appear to be any significant differences in efficacy among the older MAOIs (119), although
there are important individual differences in responsiveness, and these medications are not interchangeable.
There are no comparative studies of the newer transdermal (skin patch) formulation of selegiline; its efficacy has
only been established relative to placebo (123–125), and
clinical experience is limited.
b. Side effects of antidepressant medications
The severity of side effects from antidepressant medications in clinical trials has been assessed both through the
frequency of reported side effects and through the frequency of treatment dropout. The likelihood of different
side effects varies among classes of antidepressant medications, among subclasses, and among individual agents.
In addition, most newer antidepressants are better tolerated than TCAs (84–88, 97, 117, 126) and safer in overdose (127, 128).
When side effects occur during treatment with an antidepressant, an initial strategy is to lower the dose of the
antidepressant or to change to an antidepressant that is
not associated with that side effect. As an example, bupropion can be used if patients encounter sexual side effects
with an SSRI medication. When lowering the dose or discontinuing the medication is not effective, additional strategies may be considered. These additional strategies are
described in Table 7, which also lists prominent and clinically relevant side effects associated with particular medication classes.
Serotonin syndrome, as the name implies, is presumed
to result from high levels of serotonin in the brain. Although
it can occur with administration of one or more serotonergic medications, it is most severe when an MAOI is
coadministered with another serotonergic medication.
Consequently, great care must be taken when changing
patients from another antidepressant medication to an
MAOI and from an MAOI to other antidepressant medications because of the persistent effects of discontinued
medications. A washout period is essential before and after
using an MAOI. If the psychiatrist chooses to discontinue
a monoamine-uptake-blocking antidepressant medication
APA PRACTICE GUIDELINES
(e.g., SSRI, SNRI, TCA) and substitute an MAOI, toxic
interactions can best be avoided by allowing at least a 2-week
washout period between medication trials (Table 8). The
long half-life of the SSRI fluoxetine and its metabolites
necessitates a 5- to 6-week washout period or longer before the use of an MAOI. Additional information about
serotonin syndrome with specific medication classes can
be found in Sections II.B.2.b.1.g. and II.B.2.b.5.b.
Because knowledge of potential drug-drug interactions
is frequently changing, it is useful to consult a frequently
updated drug information database before selecting an
antidepressant in a patient taking other medications.
1. Selective serotonin reuptake inhibitors
SSRIs have comparable tolerability overall, but the specific medications differ somewhat in their side effect profiles, which may guide selection of an agent for an
individual patient. Pharmacokinetic issues, including halflife and effect on the CYP-450 enzyme system, are additional considerations in the choice of an SSRI.
a. Gastrointestinal
SSRIs commonly cause nausea, vomiting, and diarrhea
(98). These adverse events are generally dose dependent
and tend to dissipate over the first few weeks of treatment.
In some patients, however, diarrhea persists.
b. Activation/insomnia
SSRIs sometimes precipitate or exacerbate restlessness, agitation, and sleep disturbances—side effects that often
attenuate with time. Anxiety may be minimized by introducing the agent at a low dose. Akathisia has also been reported in patients taking SSRIs (129) and may contribute
to reported restlessness or activation. If akathisia does occur, a beta-blocker or benzodiazepine can be tried to reduce symptoms. Insomnia can be treated by using sleep
hygiene techniques or CBT as a first approach or by adding a sedative-hypnotic medication or trazodone. Some
have found melatonin to be helpful in treating SSRIinduced insomnia.
c. Sexual side effects
Although loss of erectile or ejaculatory function in men
and loss of libido and anorgasmia in both sexes may be
complications of virtually any antidepressant medication,
these side effects appear to be more common with SSRIs.
The psychiatrist should ascertain whether the reported sexual dysfunction is a result of the antidepressant medication,
the underlying major depressive disorder, a co-occurring
medical disorder, a disturbance in a relationship, or a need
for education about sexual functioning. If sexual dysfunction is determined to be a side effect of the antidepressant
medication, a number of strategies are available, including
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
TABLE 7.
37
Potential Treatments for Side Effects of Antidepressant Medications
Side Effect
Antidepressant Associated
With Effect
Treatmenta
Cardiovascular
Arrhythmias
TCAs
Avoid in patients with cardiac instability or ischemia.
Attend to interactions with anti-arrhythmics.
Hypertension
SNRIs, bupropion
Monitor blood pressure. Keep dose as low as possible.
Add antihypertensive.
Hypertensive crisis
MAOIs
Seek emergency treatment. If hypertension is severe,
intravenous antihypertensive agents (e.g., labetalol,
sodium nitroprusside) may be required.
Increase in cholesterol
Mirtazapine
Add a statin.
Orthostatic hypotension
TCAs, trazodone, nefazodone, Add fludrocortisone. Add salt to diet.
MAOIs
Anticholinergic
Constipation
TCAs
Encourage adequate hydration. Add bulk laxative.
Delirium
TCAs
Evaluate for other possible contributors to delirium.
Dry mouth
TCAs, SNRIs, bupropion
Suggest use of sugarless gum or candy.
Urinary hesitancy
TCAs
Add bethanechol.
Visual changes
TCAs
Add pilocarpine eye drops.
Headaches
SSRIs, SNRIs, bupropion
Assess for other etiologies (e.g., caffeinism, bruxism,
migraine, tension headache).
Myoclonus
TCAs, MAOIs
Add clonazepam.
Seizures
Bupropion, TCAs, amoxapine Assess for other etiologies, and add anticonvulsant
medication, if clinically indicated.
Neurologic
Sexual
Arousal, erectile
dysfunction
TCAs, SSRIs, SNRIs
Add sildenafil, tadalafil, buspirone, or bupropion.
Orgasm dysfunction
TCAs, SSRIs, venlafaxine,
desvenlafaxine, MAOIs
Add sildenafil, tadalafil, buspirone, or bupropion.
Priapism
Trazodone
Obtain emergency urological evaluation.
Activation
SSRIs, SNRIs, bupropion
Administer in the morning.
Akathisia
SSRIs, SNRIs
Add a beta-blocker or benzodiazepine.
Bruxism
SSRIs
Obtain dental consultation, if clinically indicated
Diaphoresis
TCAs, some SSRIs, SNRIs
Add an α1-adrenergic antagonist (e.g., terazosin), central
Other
α2-adrenergic agonist (e.g., clonidine), or
anticholinergic agent (e.g., benztropine).
Fall risk
TCAs, SSRIs
Monitor blood pressure for evidence of hypotension or
orthostasis; assess for sedation, blurred vision, or
confusion; modify environment to reduce risk.
Gastrointestinal (GI)
bleeding
SSRIs
Identify whether concomitant medications may affect
clotting.
(continued)
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38
APA PRACTICE GUIDELINES
TABLE 7.
Potential Treatments for Side Effects of Antidepressant Medications (continued)
Side Effect
Antidepressant Associated
With Effect
Treatmenta
Other (continued)
Hepatotoxicity
Nefazodone
Provide education about and monitor for clinical
evidence of hepatic dysfunction. Obtain hepatic
function tests, if clinically indicated.
Insomnia
SSRIs, SNRIs, bupropion
Use morning dosing. Add a sedative-hypnotic at
bedtime. Add melatonin. Provide CBT or education in
sleep hygiene.
Nausea, vomiting
SSRIs, SNRIs, bupropion
Administer after food or in divided doses.
Osteopenia
SSRIs
If clinically indicated, obtain bone density monitoring
and add specific treatment to reduce bone loss (e.g.,
calcium and vitamin D supplements, bisphosphonates,
selective estrogen receptor agents).
Sedation
TCAs, trazodone, nefazodone, Use bedtime dosing. Add modafinil or methylphenidate.
mirtazapine
Severe serotonin syndrome MAOIs
Obtain emergency evaluation. Consider admission to a
critical care unit.
Weight gain
Encourage exercise. Obtain input from dietician. If
changing antidepressants, consider a secondary amine
(if a TCA is required) or other antidepressant with
fewer weight issues (e.g., bupropion).
SSRIs, mirtazapine, TCAs,
MAOIs
a
Initial approaches to treatment-emergent side effects include decreasing or discontinuing the medication and changing to another
antidepressant with a different side effect profile. Treatments included here are additional measures.
continuing treatment to assess whether the dysfunction
will disappear with time, lowering the dose, discontinuing
the antidepressant, or substituting another antidepressant
such as bupropion (130). Specific pharmacological treatments that can be added for arousal difficulties, erectile
dysfunction, or orgasm dysfunction include buspirone (131),
bupropion (132), sildenafil (133), and tadalafil (134). Other
phosphodiesterase inhibitors may be also useful in treating
sexual side effects, and a variety of other medications have
been used with anecdotal success (135, 136).
d. Neurological effects
Selective serotonin reuptake inhibitors can initially exacerbate both migraine headaches and tension headaches.
These effects tend to be transient and improve within the
first few weeks of treatment. With continued treatment,
SSRIs may actually help prevent and treat migraine headaches (137, 138). Selective serotonin reuptake inhibitors
have also been associated with extrapyramidal side effects,
including akathisia, dystonia, parkinsonism, and tardive
dyskinesia (139, 140). The incidence of such side effects is
very low with SSRIs but may be higher in older patients,
especially those with Parkinson’s disease.
e.
Falls
Selective serotonin reuptake inhibitors, like other antidepressive agents, have been associated with an increased
risk of falls. In studies of nursing home residents, SSRI
use has been associated with an approximately twofold increase in the risk of a fall (141, 142). An even greater risk
of falls in patients who were taking SSRIs was noted in a
community-based cohort study (143). Meta-analyses have
also documented an increased risk of falls in patients
treated with antidepressive agents, in general (144, 145).
The implications of this increase in fall risk are complicated by the decrease in bone density that has been noted
in depressed patients (146) and in patients treated with
SSRIs (147, 148). An increase in the risk of hip fractures
has also been noted (149). Rarely, SSRI use has been associated with bradycardia, which could also contribute to
syncope and falls (150). In all patients, including those
treated with SSRIs, fall risk may be increased in individuals receiving benzodiazepines or other hypnotic agents
(144, 145, 151) and in those receiving multiple medications (144, 145). Systematically reviewing patients’ medication regimens may help to eliminate medications that
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39
Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
TABLE 8.
Required Washout Times Between Antidepressant Trials
To
MAOI
Non-MAOI
Drug with long-half-life metabolites (e.g., fluoxetine)
5–6
Drug without long-half-life metabolites (e.g., TCAs, paroxetine,
fluvoxamine, venlafaxine)
2
MAOI
2
MAOI
2
may no longer be needed, although such interventions
have not been found to alter fall risk, per se (152). Inquiring about a history of falls in the past year and assessing for
abnormalities in gait and balance can also help in identifying patients at particular risk for falling (153).
f. Effects on weight
Weight gain, at times substantial, occurs in some patients
taking SSRIs (154). Patients who take paroxetine have a
higher incidence of weight gain than those who take other
SSRIs (98, 155). Fluoxetine causes an initial reduction in
weight, which tends to normalize with continued treatment
(156).
g. Serotonin syndrome
Use of SSRIs has been associated with the rare development of a syndrome caused by an excess of central nervous
system serotonergic activity. Features of serotonin syndrome include abdominal pain, diarrhea, flushing, sweating, hyperthermia, lethargy, mental status changes, tremor
and myoclonus, rhabdomyolysis, renal failure, cardiovascular shock, and possibly death (157). Although serotonin
syndrome can occur rarely with the use of SSRIs alone, it is
usually associated with the simultaneous use of multiple
serotonergic agents and is most severe when SSRIs are given
together with MAOIs. Consequently, when an SSRI is being changed to an MAOI or vice versa, particular attention
must be give to the duration of time between treatments
(Section II.B.2.b) to avoid precipitating a potentially lethal
serotonin syndrome. Serotonin syndrome has also been reported when SSRIs are used in combination with tramadol,
high-dose triptans, or the antibiotic linezolid, which also
has some ability to inhibit MAO (158, 159).
h.
Minimum Washout Period
(weeks)
From
Drug interactions
The potential for drug-drug interactions differs significantly across the SSRIs. Selective serotonin reuptake inhibitors have variable effects on hepatic microsomal
enzymes and therefore cause both increases and decreases
in the blood levels of other medications. For example,
when SSRIs that strongly inhibit the CYP 2D6 isoenzyme
(e.g., paroxetine, fluoxetine) are administered concomitantly with tamoxifen, the metabolism of tamoxifen to its
active metabolite is reduced (76–79), resulting in a potential decrease in its efficacy in preventing breast cancer relapse (80, 81). Interaction with other drugs was higher for
fluoxetine, fluvoxamine, and paroxetine than for sertraline, citalopram, and escitalopram (98, 160, 161).
As described above, there can be a potentially lethal interaction between SSRIs and MAOIs: the serotonin syndrome. At least five half-lives should elapse between the
time an SSRI is stopped and an MAOI is started; for fluoxetine discontinuation, this means waiting approximately
5–6 weeks before starting an MAOI; for discontinuation of
other SSRIs, approximately 2 weeks should pass before
starting an MAOI (162). A 2-week waiting period has been
suggested after discontinuing an MAOI before starting an
SSRI or another MAOI (Table 8).
i.
Discontinuation syndrome
Selective serotonin reuptake inhibitors generally should
not be abruptly discontinued after extended therapy and,
whenever possible, should be tapered over several weeks
to minimize discontinuation-emergent symptoms. Clinical experience and a few controlled studies suggest that
among the SSRIs, discontinuation-emergent symptoms
are more likely with paroxetine than sertraline, citalopram, or escitalopram and least likely to occur with fluoxetine (due to the long elimination half-life of its primary
metabolite, norfluoxetine) (163, 164). Discontinuationemergent symptoms include both flu-like experiences
such as nausea, headache, light-headedness, chills, and body
aches, and neurological symptoms such as paresthesias,
insomnia, and “electric shock-like” phenomena. These
symptoms typically resolve without specific treatment
over 1–2 weeks. However, some patients do experience
more protracted discontinuation syndromes, particularly
those treated with paroxetine, and may require a slower
downward titration regimen. Another strategy is to change
to a brief course of fluoxetine, e.g., 10 mg for 1–2 weeks,
and then taper and discontinue the fluoxetine (165).
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40
2. Serotonin norepinephrine reuptake inhibitors
The most common side effects of the SNRIs (venlafaxine,
desvenlafaxine, and duloxetine) are similar to those seen
with SSRIs, including nausea and vomiting, sexual dysfunction, and activation; like the side effects seen with
SSRIs, those with SNRIs can attenuate with continued
use. The SNRIs also are more likely to be associated with
side effects that reflect noradrenergic activity, including
increased pulse rate, dilated pupils, dry mouth, excessive
sweating, and constipation. Although all three SNRIs carry
the warning of increased blood pressure, this risk is greater
during therapy with venlafaxine at doses above 150 mg/day
(166) than with duloxetine at doses of 60–120 mg/day
(167) or desvenlafaxine at doses of 50–100 mg/day (168).
Because this blood pressure increase is dose-related, SNRIinduced hypertension may respond to dose reduction. In
the absence of a reduction in hypertension, a different antidepressant medication may be considered. Alternatively,
in a patient with well-controlled depressive symptoms, it
may be preferable to add an antihypertensive agent rather
than risk a depressive relapse or recurrence with medication tapering. As with the SSRIs, abrupt discontinuation
of SNRIs should be avoided whenever possible. Discontinuation symptoms, which are sometimes protracted, are
more likely to occur with venlafaxine (and, by implication,
desvenlafaxine) than duloxetine (100) and may necessitate a
slower downward titration regimen or change to fluoxetine. As described above (Section II.B.2.b), there can be a
potentially lethal interaction between SNRIs and MAOIs:
the serotonin syndrome.
3. Other antidepressant medications
a. Bupropion
Bupropion differs from other modern antidepressants by
its lack of direct effects on serotonergic neurotransmission
and, as a consequence, a virtual lack of sexual side effects
(169). Neurologic side effects with bupropion include headaches, tremors, and seizures (106). The risk of seizures is
minimized by avoiding high doses (e.g., using no more
than 450 mg/day), avoiding rapid titration, using divided
dosing schedules for the immediate-release and sustainedrelease formulations, and avoiding use of bupropion in patients with risk factors for seizures. Bupropion should also
not be used in patients who have had anorexia nervosa or
bulimia nervosa because of elevated risk of seizures (170).
The risk of seizures may also be increased by the concomitant use of inhibitors of CYP 2B6 (e.g., desipramine,
sertraline, paroxetine, fluoxetine) due to the resulting increase in bupropion blood levels. Bupropion has been associated with a low risk of psychotic symptoms, including
delusions and hallucinations. It should therefore be used
APA PRACTICE GUIDELINES
cautiously in patients with psychotic disorders. Other
side effects with bupropion include agitation, jitteriness,
mild cognitive dysfunction, insomnia, and gastrointestinal upset.
b. Mirtazapine
The most common side effects of mirtazapine include dry
mouth, sedation, and weight gain. For this reason, mirtazapine is often given at night and may be chosen for depressed patients with initial insomnia and weight loss.
Although these side effects tend to occur early in the
treatment course and may attenuate with continued use,
the weight gain associated with mirtazapine is greater than
that with other non-TCA, non-MAOI antidepressants (95)
and may make it a less attractive choice for some patients. Mirtazapine increases serum cholesterol levels in
some patients (171). Although several patients treated
with mirtazapine were observed to have agranulocytosis
in early studies, subsequent clinical experience has not confirmed an elevated risk (172).
c. Trazodone
The most common side effect with trazodone is sedation.
Because the sedation associated with trazodone is greater
than that with other non-TCA, non-MAOI antidepressants (95), this can be an advantage in patients with initial
insomnia (173). Trazodone can also cause cardiovascular
side effects, including orthostasis, particularly among elderly patients or those with preexisting heart disease. Use
of trazodone has also been associated with life-threatening ventricular arrhythmias in several case reports
(173). Trazodone also can cause sexual side effects, including erectile dysfunction in men; in rare instances, priapism occurs, which might require surgical correction
(174, 175).
d. Nefazodone
Side effects with nefazodone include dry mouth, nausea,
constipation, orthostasis, and visual alterations (176). Sedation is also common and may necessitate a gradual
titration of nefazodone. However, in patients with insomnia, the sedating properties of nefazodone can be helpful
in improving sleep (177). There appears to be a low incidence of treatment-emergent sexual dysfunction (178,
179) with nefazodone and, unlike trazodone, it has not
been associated with priapism. Nefazodone has also been
associated with rare but potentially fatal liver failure (180,
181), which has limited its use in recent years. Drug-drug
interactions can also be problematic as nefazodone inhibits hepatic microsomal enzymes and can raise levels of
concurrently administered medications such as certain
antihistamines, benzodiazepines, and digoxin.
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
4. Tricyclic antidepressants
a.
Cardiovascular effects
Cardiovascular effects, including arrhythmias, can be
problematic with TCA treatment. Consequently, a pretreatment ECG is indicated for patients with significant
cardiac risk factors and patients older than age 50 years.
Follow-up ECGs may also be indicated to identify the development of conduction changes, typically during the
early phase of TCA use (182). Tricyclic antidepressants
act similarly to class Ia antiarrhythmic agents such as quinidine, disopyramide, and procainamide, which increase
the threshold for excitation by depressing fast sodium
channels, prolong cardiac cell action potentials through
actions on potassium channels, and prolong cardiac refractoriness through actions on both types of channels
(183). As a result, combinations of TCAs with other class
I antiarrhythmic agents can exert additive toxic effects on
cardiac conduction; patients with ventricular arrhythmias
taking another class I antiarrhythmic agent who require
TCA therapy should be under careful medical supervision. Individuals with prolonged QT intervals, whether
preexistent or medication induced, are predisposed to develop ventricular tachycardia (184). Even patients with
normal pretreatment ECG results may develop atrioventricular block with TCAs that reverts to normal after
discontinuation of antidepressant medication treatment
(185). Because of these effects on cardiac conduction,
TCAs (like other class Ia antiarrhythmic agents) may
carry an increased risk of serious cardiac adverse effects,
including mortality (186–189). In addition, fatal arrhythmias can occur in the context of TCA overdose (190, 191).
In addition to causing arrhythmias, TCAs can cause a
number of other cardiovascular side effects, including
tachycardia (through muscarinic cholinergic blockade and
α-adrenergic blockade) or orthostatic hypotension (through
α-adrenergic blockade). Side effects such as orthostatic
hypotension may in turn lead to events such as dizziness,
falls, or fractures, which are of particular concern in elderly
patients (192). Of the TCAs, nortriptyline may be less likely
to contribute to orthostatic blood pressure changes (185).
Preexisting orthostasis, antihypertensive treatment, dehydration, and salt depletion, whether voluntary or a result of diuretic treatment, may contribute to symptomatic
orthostatic hypotension with TCAs. If there is no medical
contraindication, patients with symptomatic orthostatic
hypotension should maintain adequate fluid intake and be
cautioned against extreme dietary salt restriction.
b.
Anticholinergic side effects
All TCAs have antimuscarinic effects; tertiary amine tricyclic antidepressants produce the most anticholinergic side
41
effects, whereas the secondary amines desipramine and
nortriptyline have less antimuscarinic activity (193). The
most common consequences of muscarinic blockade are
dry mouth, impaired ability to focus vision at close range,
constipation, urinary hesitation, tachycardia, and sexual
dysfunction. Although patients can develop some degree
of tolerance to anticholinergic side effects, these symptoms may require treatment if they cause substantial dysfunction or interfere with adherence. Impaired visual
accommodation may be counteracted through the use of
pilocarpine eye drops. Dry mouth may be counteracted by
advising the patient to use sugarless gum or candy and ensuring adequate hydration. Constipation can be managed
by adequate hydration and the use of bulk laxatives. Antidepressant medications with anticholinergic side effects
should be avoided in patients with cognitive impairment,
narrow-angle glaucoma, or prostatic hypertrophy. Tricyclic antidepressants can impair memory and concentration
and even precipitate anticholinergic delirium, particularly
in patients who are elderly, medically compromised, or
taking other anticholinergic medicines. Such toxic confusional states may signal the presence of high TCA blood
levels and can improve with lowering of the dose (194).
c.
Sedation
Tricyclic antidepressants also have affinity for histaminergic receptors and produce varying degrees of sedation. In
general, tertiary amines cause greater sedation, while secondary amines cause less (193). Sedation often attenuates
in the first weeks of treatment, and patients experiencing
only minor difficulty from this side effect should be encouraged to allow some time to pass before changing antidepressant medications. Patients with major depressive
disorder with insomnia may benefit from sedation when
their medication is given as a single dose before bedtime.
d. Weight gain
Tricyclic antidepressants can cause weight gain, possibly
through their histaminergic properties and/or blockade of
5-HT2 receptors (195). The degree of weight gain appears
to vary by agent (e.g., greater weight gain with amitriptyline and less with desipramine), is often dose dependent,
and is potentially reversible with cessation of TCA therapy.
Regular monitoring of weight permits early detection of
weight gain and can allow the treating clinician and patient
to determine whether a management plan to minimize or
forestall further weight gain is clinically indicated.
e. Neurological effects
Tricyclic antidepressants can cause myoclonus (196). Since
this may be a sign of toxicity, the clinician may wish to
check the blood level (if available) to ensure that it is not
excessive. If the level is nontoxic and myoclonus is not
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42
bothersome to the patient, the agent may be continued
without a change in dose. If the myoclonus is problematic and the blood level is within the recommended range,
the patient may be treated with clonazepam at a dose of
0.25 mg t.i.d. Alternatively, the antidepressant medication
may be changed. In overdoses, TCAs can cause seizures.
Some vulnerable patients may experience seizures even
on therapeutic doses of a TCA—especially clomipramine
and maprotiline (197). Amoxapine, a dibenzoxazepinederivative tricyclic antidepressant, also produces seizures
in overdose and has active metabolites that block dopamine receptors, conferring a risk of extrapyramidal side effects and tardive dyskinesia (198).
f. Falls
Use of TCAs has been associated with an increased risk of
falls in a number of studies and meta-analyses, and the relative risk of falling appears comparable to that with SSRI
treatment (141, 144, 145). Although systematic reviews
show a relatively minor effect of orthostatic hypotension on
fall risk, TCAs may contribute to orthostasis and falls in individual patients (153). If orthostatic hypotension is prominent or associated with gait or balance problems, it may
require further evaluation and treatment to minimize the
likelihood of falls (199). Other aspects of fall risk with
TCAs are similar to those that have already been described
for patients treated with SSRIs (Section II.B.2.b.1.e). Other
causes of falls include bradycardia, cardiac arrhythmia, a
seizure, or ataxia.
g. Medication interactions
A number of medications that inhibit, induce, or are metabolized by hepatic microsomal enzymes can interact
with TCAs (200). For example, medications that induce
CYP 3A4 such as carbamazepine or barbiturates will cause
a decrease in serum levels of TCAs. Drugs such as the antipsychotic medication perphenazine or SSRIs such as fluoxetine or paroxetine can inhibit metabolism via CYP
2D6, resulting in a reduced clearance and increased levels
of TCAs. Tricyclic antidepressants can also alter the pharmacokinetics or pharmacodynamics of other medications;
for example, TCAs can cause a lowering of valproate levels and reduce the activity of clonidine. Therefore, adjustments in medication doses may be necessary when TCAs
are administered concomitantly with other drugs for which
there is an interaction. The ability to obtain meaningful antidepressant blood levels to guide dosing is an advantage
with several of the TCAs (e.g., nortriptyline, amitriptyline, desipramine, imipramine) (201). Potentially dangerous interactions, including hypertensive crises and serotonin syndrome, can develop when TCAs are administered
with MAOIs (see Sections II.B.2.b and II.B.2.b.5.b), norepinephrine, or epinephrine.
APA PRACTICE GUIDELINES
5. Monoamine oxidase inhibitors
a.
Hypertensive crises
A hypertensive crisis can occur when a patient taking an
MAOI ingests large amounts of tyramine or other vasoactive amines in foods or medications (202). This reaction is
characterized by the acute onset of severe headache, nausea, neck stiffness, palpitations, profuse perspiration, and
confusion and can possibly lead to stroke and death (119).
Dietary restrictions include avoiding foods such as aged
cheeses or meats, fermented products, yeast extracts, fava
or broad beans, red wine, draft beers, and overripe or
spoiled foods (202, 203). A number of medications including norepinephrine reuptake blocking drugs (e.g., SNRIs,
TCAs), sympathomimetic vasoconstrictive agents, and overthe-counter decongestants can also produce a hypertensive crisis when used in combination with MAOIs (202,
204). Individuals with asthma who receive MAOIs should
be cautioned regarding interactions with sympathomimetic
bronchodilators, although other antiasthma agents appear to be safe. Stimulants may be added to MAOIs, but
only with caution and in selected individuals with treatmentresistant symptoms (205, 206).
At low doses (6 mg/24 hours), selegiline differs from
the older MAOIs in selectively blocking MAO B. In addition, the transdermal delivery of selegiline bypasses enzyme inhibition in the gut and first-pass metabolism in the
liver. As a result, a low-tyramine diet is not needed when
selegiline is prescribed at the minimum therapeutic dose.
However, few safety data are available at higher doses at
which selegiline becomes nonselective and inhibits both
MAO A and MAO B. Consequently, a low-tyramine diet is
needed when doses of 9 mg/24 hours and higher are prescribed as with other MAOIs (207, 208). Moclobemide,
which is available in Canada but not the United States, differs from the above MAOIs in binding reversibly to MAO
and makes dietary restrictions unnecessary with moclobemide. The potential for drug-drug interactions with selegiline and moclobemide has not been fully studied, but
caution suggests that the same drug interactions should be
considered as when prescribing the older, nonselective, irreversible MAOIs.
Although some clinicians continue to recommend that
patients carry nifedipine as a self-administered antidote
(e.g., 10 mg by mouth at the first sign of a hypertensive
crisis [209]), this practice has not been approved by the
FDA, and there are concerns about both the safety and
efficacy of this strategy, which can produce dangerous
hypotension (210). Definitive treatment of hypertensive
crises usually involves intravenous administration of an
antihypertensive agent (e.g., labetalol, sodium nitroprusside) in an emergency department setting.
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
b. Serotonin syndrome
As discussed previously in Section II.B.2.b.1.g, serotonin
syndrome is caused by excess CNS serotonergic activity
and is characterized by abdominal pain, diarrhea, flushing,
sweating, hyperthermia, lethargy, mental status changes,
tremor and myoclonus, rhabdomyolysis, renal failure, cardiovascular shock, and possibly death. Serotonin syndrome
most commonly occurs when MAOIs (including reversible
inhibitors of monoamine oxidase and selegiline) are taken
in close proximity to other serotonergic agents, such as buspirone or antidepressants (157, 204, 211). Consequently,
when patients are being changed from an SSRI other than
fluoxetine or an SNRI to an MAOI, a waiting period of at
least 2 weeks is needed between the discontinuation of one
medication and the initiation of the other. When changing
from fluoxetine to an MAOI, a waiting period of at least
5 weeks is needed before the MAOI is started (Table 8).
Other medications that have been reported to produce serotonin syndrome when used in conjunction with MAOIs
include synthetic opioids (e.g., dextromethorphan, meperidine, tramadol, propoxyphene, methadone), nonantidepressant tricyclic compounds (e.g., carbamazepine,
cyclobenzaprine), sibutramine, and over-the-counter cold
products such as chlorpheniramine (204).
c. Cardiovascular effects
Orthostatic hypotension is commonly seen during MAOI
treatment. Possible treatments for this side effect include adding dietary salt to increase intravascular volume,
or use of the mineralocorticoid fludrocortisone. Use of
MAOIs can also be associated with the development of
peripheral edema, which may be helped by the use of support stockings.
d. Weight gain
Weight gain is also commonly seen in patients treated
with nonselective MAOIs. Although clinical experience is
limited, results of one 52-week study suggested that treatment with transdermal selegiline may not be associated
with an increased risk of weight gain (212).
e. Sexual side effects
Sexual side effects seen with MAOI therapy include anorgasmia, decreased libido, and erectile or ejaculatory dysfunction. Sexual side effects may diminish over time or
with reductions in MAOI doses. The transdermal formulation of selegiline appears to have a relatively low risk of
sexual side effects (213).
f. Neurological effects
Treatment with MAOIs can also be accompanied by headaches and insomnia; these side effects may diminish over
time with continued use. Other neurological effects seen
with MAOIs include sedation, myoclonic jerks, paresthe-
43
sias, intense daytime drowsiness, and, rarely, peripheral
neuropathy.
c.
Implementation of pharmacotherapy
Improvement with pharmacotherapy can be observed as
early as the first 1–2 weeks of treatment, and improvement continues up to 12 weeks. Many patients may show
partial improvement as early as the end of the first week
(214–216). Others achieve improvement within the first
2–4 weeks (217–220). In short-term efficacy trials, all antidepressant medications appear to require at least 4–6 weeks
to achieve maximum therapeutic effects (221, 222). There
is also evidence for continued accrual of benefit for an additional 4–6 weeks (223). Furthermore, longer time to
therapeutic effect has been seen with studies conducted in
“real world” settings (224), as well as in studies of patients
with more chronic illness (225, 226) or patients with major depressive disorder complicated with co-occurring medical and/or Axis I disorders (224, 227).
Once an antidepressant medication has been selected,
it can be started at doses suggested in Table 6. Initial doses
should be incrementally raised as tolerated until a therapeutic dose is reached or the patient achieves remission,
provided there has been at least some improvement in
symptoms in the initial weeks of treatment (217–220). For
patients who exhibit a partial response to treatment, doses
of antidepressant medications should be maximized, side
effects permitting, before changing to a different antidepressant medication. In some instances, due to factors
such as rapid metabolism of medication (228, 229), patients
may require doses above those noted in FDA labeling. Patients who have achieved some improvement during the
initial weeks of treatment should be encouraged to continue taking antidepressant medication for a total of at
least 4–8 weeks. If at least moderate improvement is not
observed with maximally tolerated doses after 4–8 weeks
of treatment, reappraisal and adjustment of the pharmacotherapy should be considered. Patients with no improvement in the initial weeks of treatment generally need an
earlier adjustment of treatment. For these patients, the
psychiatrist should consider changing to another antidepressant rather than increasing the dose of the medication.
For some antidepressant medications, the exact relationships between doses and major depressive disorder symptom response have not been rigorously investigated with
fixed-dose studies, and minimum effective doses have not
been clearly established; moreover, for other antidepressant medications, some studies have failed to show doseresponse relationships (230, 231). Therefore, the initial
doses and usual adult doses in Table 6 are intended to
serve as general guidelines, and actual doses may vary
from individual to individual.
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44
Titration of the dose to full therapeutic doses generally
can be accomplished over the initial week(s) of treatment
but may vary depending on the development of side effects,
the patient’s age, and the presence of co-occurring medical
and psychiatric conditions. In general, patients who are
older, are medically compromised, or have decreased ability to metabolize and clear antidepressant medications will
require lower doses. In such patients, reduction of initial
and therapeutic doses to 50% of usual adult doses is often
recommended, and dose escalations should be made at a
slower rate than for younger and healthier adults. Doses
will also be affected by the side effect profile of medications
and the patient’s ability to tolerate these side effects. Medication doses should also be tailored to individual patients
depending on the potential for pharmacokinetic alterations
and drug-drug interactions.
Patients who have started taking an antidepressant
medication should be carefully and systematically monitored to assess their response to treatment, the emergence
of side effects, their clinical condition, safety, and adherence to treatment. Use of clinician- and patient-rated
scales can facilitate such assessments (see Section II.A.8).
Factors to consider when determining the frequency of
treatment visits include the severity of illness, the patient’s
cooperation with treatment, the availability of social supports, the presence of co-occurring general medical illnesses, and the progression of symptom change. Visits
should also be frequent enough to monitor and address
suicide risk and to actively promote treatment adherence,
since attrition from treatment continues to be a major
hurdle in maximizing outcomes. Patients in clinical trials
appear to benefit from monitoring once a week or more.
This frequency of monitoring enhances adherence rates
and likely helps patients avoid the demoralization that
may occur before the onset of beneficial effects (216). In
the recently completed STAR*D (“Sequenced Treatment
Alternatives to Relieve Depression”) trial, up to six visits
were recommended during the first 12 weeks (acute phase)
of measurement-based treatment at each of the four treatment steps (40). In clinical practice, the frequency of
monitoring during the acute phase of pharmacotherapy
may vary and can be as often as multiple times per week in
more complex circumstances. The method of monitoring
(e.g., face-to-face visits, telephone contact, or contact with
another clinician knowledgeable about the patient) may
vary depending on the clinical context and the treatment
modality.
Although for most patients, monitoring of antidepressant blood levels is not necessary, it may be useful for those
taking TCAs. For some medications, particularly nortriptyline, amitriptyline, desipramine, and imipramine, blood
drug levels correlate with both efficacy and side effects
APA PRACTICE GUIDELINES
(201, 232, 233). When such medications are given, obtaining blood drug levels can be particularly informative when
patients have not responded to treatment with an adequate
dose of antidepressant medication for an adequate duration; when patients are particularly vulnerable to the toxic
effects of a medication and require the lowest possible
effective dose; when there are concerns about patient adherence; and when there is concern that drug-drug interactions are adversely affecting antidepressant medication
levels. In time, genetic testing may help guide selection or
dosing of antidepressants, but data are currently insufficient
to justify the cost of such tests (229).
Some antidepressant medications, especially TCAs,
can cause significant morbidity and mortality in overdose
(190, 191). Ingestion of a 10-day supply of a tricyclic agent
administered at a dose of 200 mg/day is often lethal. Early
on in treatment, it is prudent to dispense only small quantities of such antidepressant medications and keep in mind
the possibility that patients can hoard medications over
time. Alternatively, in patients who are suicidal, it may be
preferable to employ agents that are safer in overdose
such as the SSRIs, bupropion, or mirtazapine.
3. Other somatic therapies
a.
Electroconvulsive therapy
Electroconvulsive therapy has the highest rates of response
and remission of any form of antidepressant treatment, with
70%–90% of those treated showing improvement (234–
236). Although the remission rate with ECT appears to be
lower when it is used in community settings than when it is
used in clinical trials (237), the proportion of patients with
major depressive disorder who respond to ECT is still
greater than the proportion who respond to antidepressant
medication. In addition, ECT has been associated with significant improvements in health-related quality of life (238).
Consequently, ECT should be considered for patients with
severe major depressive disorder that is not responsive to
psychotherapeutic and/or pharmacological interventions,
particularly those with significant functional impairment
who have not responded to numerous medication trials
(239). Electroconvulsive therapy may be particularly beneficial and can be considered as a first-line treatment option
for severe major depressive disorder when it is coupled with
psychotic features (240, 241), catatonia (239, 242), suicide
risk (243), or food refusal leading to nutritional compromise, as well as in other situations when a particularly rapid
antidepressant response is required (240), such as with severely ill inpatients (239). Electroconvulsive therapy is also
indicated as a first-line treatment for patients who have previously shown a positive response to this treatment modality
or who prefer it (239).
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
1. Side effects of electroconvulsive therapy
Electroconvulsive therapy is a very safe treatment, and
there are no absolute contraindications to its use (239).
Risks of morbidity and mortality, in general, do not exceed
those associated with anesthesia alone (239, 244, 245).
However, the presence of some medical conditions may
necessitate modifications in anesthesia or ECT administration.
Electroconvulsive therapy may have cardiovascular side
effects, mediated by changes in the autonomic nervous
system with the initial stimulus and subsequent seizure
activity (239). More specifically, ECT typically causes a
transient rise in heart rate and blood pressure, with associated increases in cardiac workload and intracranial pressure. These effects can be managed by optimizing blood
pressure control prior to ECT and administering antihypertensive agents (e.g., short-acting beta-blockers or
calcium channel blockers) at the time of ECT (239). Arrhythmias, which are usually transient, can also occur in
conjunction with ECT and can be managed with usual
antiarrhythmic therapies if they do not resolve spontaneously (239).
Electroconvulsive therapy can also be associated with
cognitive effects, the most common of which is a period of
confusion following the ECT and associated anesthesia
that generally lasts between 30 and 60 minutes (246).
Electroconvulsive therapy also is associated with anterograde amnesia, which typically resolves soon after the last
ECT treatment (247). Some degree of retrograde amnesia, particularly for recent memories, may continue for a
longer period of time after the end of the ECT course
(247) but is less pronounced for autobiographical memories than for impersonal memories (248). These cognitive
effects of ECT are related to electrode placement, stimulus
dosage, age, and premorbid cognitive status (249–253).
Retrograde amnesia also improves over time, typically resolving within 6 months (248, 252), although some patients
report incomplete recovery of memories, particularly for
events around the time of the treatment (247, 254). Rarely,
patients report more pervasive and persistent cognitive
disruption, the basis of which is uncertain (252, 255). For
many individuals, however, subjective memory (256) and
quality of life (238) is improved following ECT with the
resolution of the major depressive episode and its associated deficits in memory or executive functioning (257,
258).
2. Implementation of electroconvulsive therapy
The evaluation preceding ECT consists of a psychiatric
history and examination to verify that ECT is indicated, a
general medical evaluation (including medical history and
physical examination with cognitive assessment, vital signs,
45
and any specifically indicated laboratory, radiologic, or
imaging studies) to define factors that may influence the
risk of ECT, and an anesthesia evaluation to identify and
address the nature and extent of anesthetic risk and the
need for modification of medications or anesthetic technique (239). This evaluation should include a summary of
treatment indications, treatment risks, and a suggestion of
any indicated additional evaluative procedures, alterations
in treatment, or modifications in ECT technique (239). In
assessing indications for caution (e.g., recent myocardial
infarction, cardiac arrhythmias, intracranial space-occupying lesions), the relative risks and benefits should be
carefully weighed in collaboration with an anesthesiologist, a general medical physician, and other specialists, as
necessary. Once completed, the pre-ECT evaluation will
serve as the basis for a specific, individualized discussion
of the risks and benefits of ECT relative to other therapeutic options as part of the informed consent process.
With the patient’s permission, it is helpful to educate the
patient’s family about ECT and involve them in discussions relating to consent.
An additional aspect of decision-making prior to ECT
relates to the use of psychotropic medications during the
ECT course. There is growing use of ECT combined with
antidepressant medication. Although data supporting this
practice are still few, it does not appear to increase side effects and may augment response (259, 260). An additional
goal of combination treatment is to minimize the risk of
relapse between the end of the ECT course and the attainment of full antidepressant effectiveness. Antipsychotic
medications are typically continued during the ECT
course (239, 261), although most data on this practice come
from studies of patients with schizophrenia who are receiving ECT. The safety of combining lithium and ECT
has been questioned, although there are conflicting data
(239, 262). Medications that have anticonvulsant properties are often discontinued or given at decreased doses
during the ECT course to minimize effects on seizure induction (239, 261). With benzodiazepines, there is some
evidence that concurrent use may diminish ECT effectiveness, particularly when right unilateral electrode placement is used (263).
Electroconvulsive therapy may be administered either
unilaterally or bilaterally (using a bitemporal or bifrontal
electrode placement). Compared with patients who receive bilateral treatment, most patients who receive right
unilateral electrode placement with low stimulus intensities experience fewer cognitive effects but less therapeutic
benefit (253). Stimuli of higher intensity (i.e., 500% above
seizure threshold) are associated with antidepressant effects more comparable to those seen with bilateral electrode placements, although such stimulus intensities are
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46
APA PRACTICE GUIDELINES
not always achievable with existing ECT devices (264). Regardless of what electrode placement is chosen, stimulus
dosing should be individualized and stimulus parameters
adjusted to induce an adequate generalized seizure, which
is typically at least 20 seconds or greater in motor duration
and 30 seconds in EEG duration (239). Failure to induce
an adequate seizure should be followed immediately by
restimulation at higher energies until an adequate seizure
is elicited.
Electroconvulsive therapy is typically administered
2–3 times/week; less frequent administration has been associated with less cognitive impairment but also a longer
lag in the onset of action (265). In clinical practice, the
need for ECT to be administered at this frequency could
produce logistical barriers for some patients who would
either require hospitalization or transportation after ECT
sessions. The acute course of ECT treatment typically
consists of six to 12 treatments and generally does not exceed 20 treatments (239, 266). It is important that treatment continue until symptoms have remitted or clearly
reached a plateau, since relapse rates appear to be greater
and overall prognosis worse if ECT is discontinued prematurely (237). Use of a formal rating scale may be helpful in assessing symptom response as well as the cognitive
side effects of treatment, permitting adjustments in the
treatment parameters or frequency (239, 267).
For more detail on the administration of ECT, see APA’s
The Practice of Electroconvulsive Therapy: Recommendations
for Treatment, Training, and Privileging (A Task Force Report
of the American Psychiatric Association) (239).
b.
Transcranial magnetic stimulation
Transcranial magnetic stimulation (TMS) uses a specifically
designed magnetic coil that is placed in contact with the
head to generate rapidly alternating magnetic-resonanceimaging-strength magnetic fields and produce electrical
stimulation of superficial cortical neurons. Based on the
results of a multisite randomized sham-controlled clinical
trial of high-frequency TMS over the left dorsolateral
prefrontal cortex (268), TMS was cleared by the FDA in
2008 for use in individuals with major depressive disorder
who have not had a satisfactory response to at least one
antidepressant trial in the current episode of illness. However, another large randomized sham-controlled trial of
TMS added to antidepressant pharmacotherapy showed
no significant benefit of left dorsolateral prefrontal cortex
TMS (269). In comparisons of actual TMS versus sham
TMS, most (270–272) but not all (273) recent meta-analyses have found relatively small to moderate benefits of
TMS in terms of clinical response. Although the primary
studies used in these meta-analyses are highly overlapping
and the variability in TMS stimulus parameters and treat-
ment paradigms complicates the interpretation of research findings, these meta-analyses also support the use
of high-frequency TMS over the left dorsolateral prefrontal cortex. Lesser degrees of treatment resistance may
be associated with a better acute response to TMS (274).
In comparison with ECT, TMS has been found in randomized studies to be either less effective than ECT (275)
or comparable in efficacy to ECT (276–278), but in the
latter studies TMS was more effective and ECT was less
effective than is typically seen in clinical trials. A fewer
number of studies have compared cognitive effects of
TMS and ECT. One randomized trial found no significant difference between TMS and non-dominant unilateral ECT on performance on neuropsychological tests
at 2 and at 4 weeks of treatment (276), although a small
open-label trial reported a greater degree of memory difficulties with ECT than with TMS shortly after the treatment course (279).
Across all studies, TMS was well tolerated and was associated with low rates of treatment dropout (270, 280).
Transient scalp discomfort and headaches were the most
commonly reported side effects (280).
In clinical practice, the need for daily TMS could produce logistical barriers for some patients.
c. Vagus nerve stimulation
Vagus nerve stimulation is approved for use in patients
with treatment-resistant depression on the basis of its potential benefit with long-term treatment. There is no indication for the use of VNS in acute phase treatment of
depression, as data showed no evidence for acute efficacy
(281, 282). Further information on the use of VNS as an
adjunct to other antidepressive treatments is provided in
Section II.B.7.c.
4. Psychotherapy
There has been considerable research on time-limited
psychotherapies for major depressive disorder, although
the number of studies is smaller than for pharmacotherapies. Most research has focused on individual, in-person,
outpatient treatment, in part based on the needs and constraints of research methods. However, research has also
begun to explore psychotherapies in differing formats,
including groups, over the telephone, and with computer
assistance.
When psychotherapy is part of the treatment plan, it
must be integrated with psychiatric management (Section
II.A) and any other treatments (e.g., pharmacotherapy) that
are being provided. Clinical considerations and other
patient factors should be considered in determining the
nature and intensity of psychotherapy. Typically psychotherapy is given in an ambulatory setting, although some
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
psychotherapies might benefit depressed inpatients, given
adequate lengths of stay and courses of treatment (283–
285). Like pharmacotherapy, the effectiveness of psychotherapy will vary with the skill and training of the therapist.
Patient factors, such as the nature and duration of depressive symptoms, beliefs and attitudes toward psychotherapy,
and early life experiences (e.g., history of trauma) also affect
treatment response to psychotherapy. Psychotherapy is
particularly useful in addressing the psychosocial stressors
and psychological factors that have an impact on the development or maintenance of depressive symptoms.
Cognitive-behavioral therapy, interpersonal psychotherapy (IPT), and behavioral psychotherapies (e.g., behavioral activation) have demonstrated acute efficacy in
treating major depressive disorder. There is less evidence
for other psychotherapies. However, one meta-analysis
found no large differences in long-term efficacy between
any of the major psychotherapies, including dynamic psychotherapy, for mild and moderate depression (286). In
terms of longer term outcomes, psychotherapy is generally
found to have more prolonged effects than pharmacotherapy after cessation of active treatment. In particular, IPT
and CBT have shown lasting benefits in maintaining remission (287–289). These time-limited treatments are essentially equipotent with antidepressant medications for
outpatients with mild to moderate acute depression but
probably should be used in conjunction with medication
for severe or melancholic major depressive disorder. Some
research has suggested patient and illness characteristics
that might predict differential benefits of CBT over IPT,
and vice versa, for patients with major depressive disorder
(e.g., see reference 290), but such preliminary findings require replication.
Cognitive-behavioral therapy and IPT appear less effective than pharmacotherapy for chronic depression, at
least as acute monotherapy (291–296). Nonetheless, in
patients who respond to medication, psychotherapy may
foster the development of social skills and confidence after years of depression-related impairments (297).
Psychotherapy carries its own “side effects.” A psychotherapy that requires considerable time or patience may
be poorly tolerated. The work of psychotherapy itself may
generate anxiety or other strong feelings, which may be
difficult for patients to manage. An indirect measure of
the relative side effects and tolerability of psychotherapy
can be obtained from the dropout rates in clinical trials;
however, many other factors can also affect these rates
(e.g., other burdens of the research trial, specific features
of the clinical management provided, logistical barriers in
attending appointments). Depending on what can reasonably be expected with the given type of psychotherapy, the
psychiatrist should consider a change in the intensity or
47
type of psychotherapy and/or addition or change to medication if psychotherapy for major depressive disorder has
not resulted in significant improvement in 4–8 weeks.
a.
Specific psychotherapies
1. Cognitive and behavioral therapies
In the treatment of depressed patients, psychotherapies
that focus primarily on aspects of cognitive patterns and
those that emphasize behavioral techniques can be used
alone, but are generally used in combination. Cognitivebehavioral therapy combines cognitive psychotherapy
with behavioral therapy and maintains that irrational
beliefs and distorted attitudes toward the self, the environment, and the future perpetuate depressive affects and
compromise functioning. The goal of CBT is to reduce
depressive symptoms by challenging and reversing these
beliefs and attitudes and encouraging patients to change
their maladaptive preconceptions and behaviors in real
life (298).
Cognitive-behavioral therapy is an effective treatment
for major depressive disorder. In meta-analyses, CBT has
generally surpassed control conditions in efficacy and has
had equal efficacy compared with other empirically supported psychotherapies (i.e., IPT and behavior therapy)
(299). Studies comparing the effectiveness of CBT with
pharmacotherapy, however, are methodologically challenging to conduct, and results are inconsistent (296, 300).
Also unclear is whether CBT is less effective for patients
with more severe depressive symptoms.
Behavior therapy for major depressive disorder is based
on theoretical models drawn from behavior theory (301)
and social learning theory (302). Behavioral activation is a
newly articulated behavioral intervention with some positive preliminary results that merit further study (288,
303). Specific behavior therapy techniques include activity scheduling (304, 305), self-control therapy (306),
social skills training (307), and problem solving (308). Behavior therapy involves graded homework, scheduling of
enjoyable activities, and minimizing unpleasant activities
(309). Behavior therapy has demonstrated efficacy, at times
superior to cognitive therapy, in treating major depressive
disorder (310).
2. Interpersonal psychotherapy
The focus of IPT is on current life changes, including
losses, role disputes and role transitions, social isolation,
deficits in social skills, and other interpersonal factors that
may interact with the development of the depressive
episode (311, 312). In IPT the goal is to intervene by identifying the current trigger of the depressive episode, facilitating mourning in the case of bereavement, promoting
recognition of related affects, resolving role disputes and
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48
role transitions, and building social skills to improve relationships and to acquire needed social supports. In IPT,
major depressive disorder is defined as a medical illness,
and the illness, rather than the patient, is blamed for the
symptoms. Interpersonal psychotherapy’s medical model
makes it highly compatible with pharmacotherapy in
combined treatment.
Interpersonal psychotherapy is an efficacious treatment for major depressive disorder (296, 313). Studies
have shown efficacy of this treatment in depressed primary care patients and patients with more severe depression (311). The efficacy of IPT has been demonstrated for
adolescents, pregnant and postpartum women, and geriatric patients (311). Interpersonal psychotherapy can also
be used as a monthly maintenance therapy to prevent
relapse (289, 314, 315). Some studies have also suggested
possible subgroups in whom IPT may show differential
efficacy, specifically among HIV-positive patients (316)
and patients who have co-occurring obsessive personality
traits and who are single and not living with others (317).
Furthermore, for patients with severe life events, IPT may
have advantages over therapies that do not focus on such
events directly.
3. Psychodynamic psychotherapy
The term “psychodynamic psychotherapy” encompasses a
range of brief to long-term psychotherapeutic interventions (318–320). These interventions derive from psychodynamic theories about the etiology of psychological
vulnerability, personality development, and symptom formation as shaped by development and conflict occurring
during the life cycle from earliest childhood forward (321–
325). Some of these theories focus on conflicts related to
guilt, shame, interpersonal relationships, the management
of anxiety, and repressed or unacceptable impulses. Others
address developmental psychological deficits produced by
inadequacies or problems in the relationship between the
child and emotional caretakers, resulting in problems of
self-esteem, sense of psychological cohesiveness, and emotional self-regulation (323, 326–330).
Psychodynamic psychotherapy may be brief but usually has a longer duration than other psychotherapies, and
its aims extend beyond immediate symptom relief. These
goals are to modify underlying psychological conflicts and
deficits, which increase the patient’s vulnerability to depressive affect and the development of major depressive disorder. Psychodynamic psychotherapy is therefore broader
than most other psychotherapies, encompassing both current and past problems in interpersonal relationships,
self-esteem, and developmental conflicts associated with
anxiety, guilt, or shame. Time-limited, structured psychodynamic psychotherapy may focus more on understand-
APA PRACTICE GUIDELINES
ing the psychological basis of the presenting symptoms or
on a selected underlying conflict. Sometimes a goal of psychodynamic psychotherapy, brief or extended, may be to
help the patient accept or adhere to necessary pharmacotherapy (331).
Although psychodynamic psychotherapy is often used
in clinical practice, its efficacy in the acute phase of major
depressive disorder remains less well studied in controlled
trials than the efficacy in this phase of some other forms of
psychotherapy. This research is reviewed in Part B, Section V.B.3.
4. Problem-solving therapy
Problem-solving therapy is a manual-guided, brief treatment lasting six to 12 sessions. This therapy, often administered by nurses or social workers, has been used to
prevent depression in elderly and/or medically ill patients,
and it has also been used to treat patients with relatively
mild depressive symptoms. The approach combines elements of cognitive therapy (addressing negative assessments of situations) and IPT (focal problem solving). Some
studies have reported modest improvement in patients
with mild depressive symptoms. Although problem solving therapy has had limited testing for patients with major
depressive disorder, it may have a role in targeted patient
populations with mild depression (332–335).
5. Marital therapy and family therapy
Marital and family problems are common in the course of
mood disorders, and comprehensive treatment often demands assessing and addressing these problems. Marital
and family problems may be the consequence of major depressive disorder but may also increase vulnerability to
developing major depressive disorder or retard recovery
from it (336–339). A number of marital and family therapies have been shown to be effective in the treatment
of depression. Techniques include behavioral approaches
(338), problem-focused approaches (340), and strategic
marital therapy (341, 342). Family therapy has also been
found to be helpful in the treatment of more severe forms
of depression in conjunction with medications and hospitalization (343).
6. Group therapy
Group psychotherapy is widely practiced, but research on
its application to major depressive disorder is limited.
Specific types having some data to support their efficacy
include CBT (344–347) and IPT (348–351). Meta-analyses
of the relative effectiveness of psychotherapeutic approaches
conducted in group format versus individual format have
not involved patients with rigorously defined major depressive disorder (352–355).
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
On the basis of a very limited controlled study, supportive group therapy has been suggested to have utility in the
treatment of major depressive disorder. In a study of depressed outpatients, a mutual support group and group
CBT were found to be equally effective in reducing depressive symptoms (346). In a study of HIV-positive patients with mild to moderate major depressive disorder,
structured supportive group therapy plus placebo yielded
similar decreases in depressive symptoms to structured
group therapy plus fluoxetine (356). Individuals experiencing stressors such as bereavement or chronic illness may
benefit from contact with others facing similar challenges.
Medication maintenance support groups may also offer benefits, although data from controlled trials for patients with major depressive disorder are lacking. Such
groups inform the patient and family members about
prognosis and medication issues, providing a psychoeducational forum that contextualizes a chronic mental illness
in a medical model.
The efficacy of self-help groups led by lay members
(357) in the treatment of major depressive disorder has
not been well studied. However, one investigation of
group therapies found that a higher proportion of depressed outpatients had remission following treatment in
groups led by professionals than had remission following
participation in groups led by nonprofessionals (346).
Further study is needed on the possibility that self-help
groups may serve a useful role in enhancing the support
network and self-esteem of participating patients with
major depressive disorder and their families.
Overall, group therapy has some evidence to support
its use as well as the potential advantage of lowered cost,
inasmuch as one or two therapists can treat a larger number of patients simultaneously. This advantage needs to be
weighed against the difficulties in assembling the group,
the lesser intensity of focus patients receive relative to individual psychotherapy, and potentially adverse effects
from interactions with other group members.
b. Implementation
It can be useful to establish an expected duration of psychotherapy at the start of treatment. Communicating this
expectation may help mobilize the patient and focus treatment goals, yet there are few data available on the optimal
duration of specific depression-focused psychotherapies.
In many trials, CBT and IPT have been delivered in approximately 12–16 weekly sessions. In a subanalysis of one
clinical trial, CBT delivered in 16 weeks was more effective than CBT delivered in 8 weeks for those with severe
major depressive disorder (358). Moreover, evidence suggests benefit from monthly continuation phase treatment
with IPT in reducing the probability of relapse (314). In
49
addition, patients with chronic, treatment-resistant depression may require long-term treatment.
The optimal frequency of psychotherapy has not been
rigorously studied in controlled trials. The psychiatrist
should consider multiple factors when determining the
frequency for individual patients, including the specific
type and goals of the psychotherapy, the frequency necessary to create and maintain a therapeutic relationship, the
frequency of visits required to ensure treatment adherence, and the frequency necessary to monitor and address
suicide risk and other safety concerns. Time-limited brief
psychotherapies may mobilize many depressed patients to
more rapid improvement. The severity of illness, the patient’s cooperation with treatment, availability of social
supports, cost, geographic accessibility, and presence of
co-occurring general medical problems may also influence visit frequency. The frequency of outpatient visits
during the acute phase is generally weekly but may vary
based on these factors. Some experienced clinicians find
that sessions are needed at least twice weekly, at least initially, for patients with moderate to severe depression.
Regardless of the type of depression-focused psychotherapy that is selected, the clinician should carefully and
systematically monitor the patient’s response to treatment,
which can be facilitated by the use of clinician- and patientrated scales at regular intervals (see Section II.A.8). If 4–8
weeks of treatment do not yield at least moderate improvement (≥20% diminution in symptoms), the clinician
should thoroughly review and reappraise the treatment
plan.
c.
Combining psychotherapy and medication
Several meta-analyses of studies of the combination of
psychotherapy and pharmacotherapy for patients with
major depressive disorder have documented a modest advantage for the combination as compared with one or the
other modality alone (359–361). Particularly large additive effects have been observed in individual studies of patients with chronic depression (362), patients with severe
recurrent depression (359), and hospitalized patients
(285). Combined treatment might therefore be considered a treatment of first choice for patients with major depressive disorder with more severe, chronic, or complex
presentations. Combining family therapy with pharmacotherapy has also been found to improve posthospital care
for depressed patients (343).
Dual treatment combines the unique advantages of each
therapeutic modality: while pharmacotherapy may provide
earlier symptomatic relief, psychotherapy yields broader
and longer lasting improvement (363). Psychotherapy can
also be used to address issues that arise during pharmacotherapy, such as decreased adherence. However, the advan-
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
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50
tage of routinely combining interventions may be modest
for patients with less severe depressive symptoms (359).
There are no empirical data from clinical trials to help
guide the selection of particular antidepressant medications
and particular models of psychotherapeutic approaches
for individuals who will receive the combination of both
modalities. In general, the same issues that influence these
decisions when choosing a monotherapy will apply, and
the same doses of antidepressant medication and the same
frequency and course of psychotherapy should be used for
patients receiving combination modality treatments as are
used for patients receiving them as a monotherapy.
Results from a series of recent studies provide indirect
evidence that for patients who have had only a partial response to pharmacotherapy, adding a course of CBT may
be an effective strategy for preventing relapse (363–368).
During 12 weeks of treatment in the STAR*D study, cognitive therapy was as effective as either augmenting with
bupropion or buspirone or changing antidepressants to
bupropion, sertraline, or venlafaxine. However, patients
who did not respond to an initial course of citalopram were
less likely to accept cognitive therapy as a change or augmentation option than they were to accept a different medication option (369), perhaps due to the nature of the study
design.
5. Complementary and alternative treatments
As defined by the National Center for Complementary
and Alternative Medicine, complementary and alternative
medicine is “a group of diverse medical and health care
systems, practices, and products that are not presently considered to be part of conventional medicine.” As the definitions are usually applied, “complementary” therapies are
used conjunctively with conventional medicine, “alternative” therapies are used in place of conventional medicine,
and “integrative” medicine makes use of all therapies appropriate to an individual patient’s needs.
The use of integrative therapies is increasingly common, although training and comfort with complementary
and alternative modalities vary greatly by practitioner.
Many patients do not spontaneously disclose use of complementary or alternative treatments to health care professionals, so it is particularly important that direct inquiry about
such treatments be part of routine health care questions.
At this time, there are several modalities that have modest evidence for antidepressant efficacy and deserve
further study. Some of these modalities can be recommended with enthusiasm for their general health benefits;
however, patients should be informed that evidence for
their antidepressant efficacy as monotherapy is limited or
absent.
APA PRACTICE GUIDELINES
a. St. John’s wort
St. John’s wort is a plant widely used to treat depressive
symptoms. Overall, studies of St. John’s wort show greater
consensus and support for benefits in mild to moderate major depressive disorder, as compared with less consistent
findings in patients with more severe symptoms. One review of 14 short-term, double-blind trials conducted in
outpatients with mild to moderate symptoms of major depressive disorder concluded that St. John’s wort in doses of
300 mg/day and 1,800 mg/day had efficacy that was superior to placebo (105). St. John’s wort had generally comparable efficacy and fewer side effects than low-dose TCA
treatment (e.g., 30–150 mg/day of amitriptyline) (105), but
doses at the low end of this range would not be expected to
produce therapeutic benefits. However, in the two largest
controlled studies conducted in the United States (370,
371), effects of St. John’s wort did not differ from placebo,
which somewhat limits confidence in the magnitude of the
antidepressant actions of St. John’s wort. In addition, preparations of St. John’s wort are not regulated by the FDA as
a drug and lack standardization of their ingredients, composition, and potency. Based on the evidence cited, St.
John’s wort would not meet the FDA’s minimum requirements to be declared an effective antidepressant and is not
recommended for general use in treating depression.
Another important consideration with St. John’s wort
is the potential for drug-drug interactions (372–374). St.
John’s wort appears to induce the metabolism of drugs via
CYP 3A4, reducing the efficacy of medications, including
antiretroviral medications, immunosuppressants (including cyclosporine), antineoplastic agents, anticoagulants
(including warfarin), oral contraceptives, and hormone
replacement therapy (373, 374). Unwanted pregnancies
have been reported with concomitant St. John’s wort and
oral contraceptive use (373, 375, 376), and rejection of transplanted organs has been observed when St. John’s wort is
taken concurrently with cyclosporin (374). The significant
decreases in antiretroviral medication levels with concomitant St. John’s wort use suggest that these medications will be less effective in treating HIV infection (374).
Effects of St. John’s wort on P-glycoprotein have also been
observed, altering the pharmacokinetics and pharmacodynamics of medications such as digoxin that are transported by this route (374). Apart from affecting blood
levels of nonpsychiatric medications, the safety and efficacy of the combined use of St. John’s wort with other antidepressant medications is not known. The combined use
of St. John’s wort with MAOIs is contraindicated.
b. S-adenosyl methionine
S-adenosyl methionine is a naturally occurring molecule.
In humans, it is concentrated in the liver and the brain and
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
serves as a methyl donor in the synthesis of biologically
active compounds such as phospholipids, catecholamines,
and the neurotransmitters dopamine and serotonin (377).
Cerebrospinal fluid levels of SAMe are lower in individuals with severe major depressive disorder, compared with
control subjects (378), and treatment with SAMe increases
CSF SAMe and 5-hydroxyindoleacetic acid levels (379).
S-adenosyl methionine is available for both parenteral and
oral administration (380).
Some data support the efficacy and tolerability of SAMe
in patients with major depressive disorder. Oral, intravenous, and intramuscular formulations have been assessed
and appear efficacious in at least pilot studies (381–383).
Like St. John’s wort, SAMe is not regulated by the FDA
and lacks standardization of its composition and potency.
S-adenosyl methionine has been compared with TCAs
and has been reported to have greater efficacy while being more tolerable (381). It is unclear at present how
SAMe compares to SSRIs in efficacy and cost-efficiency.
While some data support the use of SAMe as monotherapy and as augmentation therapy, the data at this time, as
with St. John’s wort, are insufficient to make a recommendation for its use in the treatment of major depressive disorder.
c. Omega-3 fatty acids
Most studies of omega-3 fatty acids for major depressive
disorder have been adjunctive studies, in which patients
were already receiving antidepressant medications but still
met the criteria for major depressive disorder. Studies vary
in the omega-3 fatty acids used (eicosapentaenoic acid
[EPA], docosahexaenoic acid [DHA], or the combination),
and doses and durations of study trials have also varied. It is
difficult to interpret the literature on this treatment given
the heterogeneity in study design and outcomes.
Omega-3 fatty acids are generally recommended as an
adjunctive therapy for mood disorders, as health benefits,
including those for cardiovascular health, are well established, and individuals with psychiatric disorders may
be at greater risk for obesity, metabolic problems, and
other health problems than the general population (384,
385). More evidence is required to establish a definitive
role in the acute treatment of major depressive disorder.
Doses of 1–9 grams have been studied in mood disorders,
with a majority of evidence supporting use of lower
doses. Adjunctive EPA or the combination of EPA and
DHA (the combination found in most commercially
available brands) appears most useful, with less evidence
for DHA alone for the treatment of major depressive
disorder. Further data are needed to ascertain the role of
omega-3 fatty acids as monotherapy for major depressive
disorder.
d.
51
Folate
Folate has been primarily assessed as a predictor of antidepressant medication response and as an adjunctive
treatment. Low folate blood levels have been associated
with lack of response and slower response to fluoxetine for
major depressive disorder (386, 387), and higher folate
levels at treatment baseline appear associated with better
response to antidepressants (388). Folate has been studied
as an adjunctive treatment compared with placebo in addition to fluoxetine, with significantly greater improvement in those receiving folate, especially among female
patients (389).
Folate is a low-risk intervention with general health
benefits. Folate protects against neural tube defects in
early pregnancy. In general, 0.4–1 mg of folate is recommended for women of reproductive age. Considering the
modest evidence that supports folate as an augmentation
strategy and its attractive risk-benefit profile, folate can
be recommended as a reasonable adjunctive strategy for
major depressive disorder that carries little risk and may
decrease birth defects in the case of pregnancy. Data are
inadequate to suggest efficacy as a monotherapy.
e. Light therapy
Bright light therapy appears effective for seasonal affective disorder and nonseasonal major depressive disorder, as demonstrated in generally short-term, placebocontrolled trials (390–394), although some studies have
methodological limitations (395). The mechanism of action for light therapy is not clear but appears to involve
the serotonergic neurotransmitter system (396, 397).
There is some evidence that light therapy may hasten the
response to treatment with antidepressant medication
(398). Open-label data also support light therapy for patients
with major depressive disorder that has not responded to
antidepressant medication (399). Greater intensity of light
is associated with efficacy (400). Light therapy also may
augment the antidepressant benefits of partial sleep deprivation (401, 402). Monitoring for mania and hypomania
may be appropriate with initiation of light therapy, as hypomania has been reported (392). However, in general
bright light therapy is a low-risk and low-cost option for
treatment.
f. Acupuncture
Acupuncture is a treatment modality that is part of traditional Chinese medicine. Its efficacy is somewhat difficult
to assess, as much of the research is published in Asian languages and overlooked in typical literature searches. In
addition, there is significant variation in the acupuncture
techniques used as well as limited descriptions of methodology and diagnosis (403). One randomized trial showed
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52
comparable benefits of electroacupuncture and amitriptyline (404), and another small randomized trial in depressed
women showed benefits of acupuncture relative to a sham
control (405). However, a subsequent larger study did not
replicate these results (406), and a recent meta-analysis
concluded that acupuncture was not associated with any
benefits in treating major depression in terms of response
or remission rates (407). Assuming needles are properly
sterilized, there do not appear to be substantial risks of
acupuncture treatment. However, based on current evidence, acupuncture is not recommended in the treatment
of major depressive disorder.
APA PRACTICE GUIDELINES
TABLE 9.
Potential Reasons for Treatment Nonresponse
Inaccurate diagnosis
Unaddressed co-occurring medical or psychiatric
disorders, including substance use disorders
Inappropriate selection of therapeutic modalities
Inadequate dose of medication or frequency of
psychotherapy
Pharmacokinetic/pharmacodynamic factors affecting
medication action
Inadequate duration of treatment
Nonadherence to treatment
Persistent or poorly tolerated side effects
6. Assessing response and adequacy of treatment
Complicating psychosocial and psychological factors
The goal of acute phase treatment for major depressive disorder, insofar as possible, is to achieve remission and a return to full functioning and quality of life. Remission is
defined as at least 3 weeks of the absence of both sad mood
and reduced interest and no more than three remaining
symptoms of the major depressive episode (408). However,
it is not uncommon for patients to have substantial but incomplete symptom reduction or improvement in functioning during acute phase treatment. A number of studies have
provided compelling evidence that even mild residual
symptoms at the end of a depressive episode are associated
with significant psychosocial disability, compared with asymptomatic remission (409); a more than three times faster
relapse to a subsequent major depressive episode (410); and
in first-episode patients, a more chronic future course (410–
412). The presence of mild residual symptoms has been
shown to be an even stronger predictor of a subsequent return to a major depressive episode than a prior history of
multiple episodes of major depressive disorder (410). For
this reason, it is important not to conclude the acute phase
of treatment prematurely for partially responsive patients.
Throughout treatment, both the patient’s response and the
adequacy of treatment must be vigilantly and systematically
monitored. Use of structured measures of depression
symptom severity, side effects, treatment adherence, and
functional status can facilitate identification of patients who
have not had a complete response to treatment (40, 44).
If a patient is found to have an incomplete treatment
response, the treatment itself should be evaluated. Medications must be thoughtfully selected and given at an adequate dose and for an adequate duration. Similarly,
psychotherapy must be well chosen for the patient, skillfully executed, and conducted over an appropriate period
of time with an adequate frequency of visits. In addition to
being caused by inadequate treatment, poor response may
result from multiple other factors (413) that are enumerated in Table 9.
Inadequately trained therapist or poor “fit” between
patient and therapist
For pharmacotherapy, determination of the adequacy of
treatment requires ensuring that antidepressant medications have been used for an adequate dose and duration.
This can be assessed using standardized measurement instruments (414). Generally, adequate treatment with an
antidepressant medication for at least 4–6 weeks is necessary before concluding that a patient is not responsive or
only partially responsive to a particular medication (218,
221). For patients with no improvement in symptoms
during the initial weeks of treatment, treatment should be
reevaluated and possibly changed. Furthermore, there is
little evidence to support extending antidepressant medication trials beyond 6 weeks in patients who have shown
no response. Patients with chronic forms of depression or
with co-occurring Axis I disorders or general medical
conditions may require a longer duration of acute phase
treatment before concluding that a different treatment
strategy is indicated (224).
For psychotherapy, treatment should be reassessed if
there has not been meaningful improvement after a few
months, depending on what can reasonably be expected for
the given type of psychotherapy. Patients should be reassessed every 3–4 months to ensure adequate improvement.
Regardless of treatment modality, lack of improvement
over time warrants reconsideration of interventions, given
the large number of available treatment options.
7. Strategies to address incomplete response
The psychiatrist should consider a change in treatment
for patients who have not fully responded to an adequate
acute phase treatment over a sufficient time, generally
4–8 weeks. The treatment plan can be revised by implementing one of several therapeutic options, including op-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
53
Response
None or Partial
Full
Initial weeks
If treatment is well-tolerated, maintain
Assess adherence. If clinical severity
current treatment approach.
warrants and treatment is well tolerated,
consider increasing medication dosage or
intensity of psychotherapy, especially if
there is no response. If symptoms are
severe or life-threatening, consider ECT.
At 4–8 weeks
In patients treated with an antidepressant, Go to continuation phase.
consider increasing the dose (if well
tolerated), changing to a different
antidepressant, and changing to or
augmenting with psychotherapy.
Augmentation therapy or ECT may
also be considered.
For insufficient response to psychotherapy,
consider changing the intensity or type
of psychotherapy and/or adding or
changing to medication.
For ECT, see guideline text.
Throughout treatment
In patients who have significant side effects with antidepressant treatment, consider
changing to a different antidepressant, reducing the dose, or treating the side effect.
Also consider changing to psychotherapy or ECT.
If trials of two medications from the same antidepressant class have been ineffective,
consider changing antidepressants to a different class.
For patients with difficulty tolerating psychotherapy, consider changing the intensity or
type of therapy and/or adding or changing to medication.
FIGURE 2.
Assessment of Treatment Tolerability and Adequacy of Response
timizing the initial treatment, changing to a different
treatment, and combining treatments. These options are
outlined in Figure 2 and described in more detail below.
Following any change in treatment, the patient should
continue to be closely monitored. If there is not at least a
moderate improvement in major depressive disorder
symptoms after an additional 4–8 weeks of treatment, the
psychiatrist should conduct another thorough review. This
reappraisal should include the following: verifying the patient’s diagnosis and adherence; uncovering and addressing clinical factors that may be preventing improvement,
such as the presence of co-occurring general medical conditions or psychiatric conditions (e.g., alcohol or substance
abuse); evaluating for potential drug-drug interactions;
obtaining collateral information from those involved with
the patient; and uncovering and addressing psychosocial,
psychological, and personality factors that may be impeding recovery (Table 9). If no new information is uncovered
to explain the patient’s lack of adequate response, other
treatment options should be considered, including ECT
and a consultation from an expert in mood disorders. Despite optimal treatment, some patients may continue to
have chronic depressive symptoms. For these patients, the
psychiatrist should add a disease management component
to the overall treatment plan. This component involves
setting realistic expectations, improving functioning, and
developing self-management skills (415, 416).
a. Maximizing initial treatments
For patients who have not fully responded to treatment
for depression, an initial strategy is to optimize the intensity of psychotherapy or maximize the dose of medication,
especially if the upper limit of the antidepressant dose has
not been reached. Decisions about pharmacotherapy will
involve a balancing of efficacy, side effects, and medication adherence. Dose escalation and management of side
effects at critical decision points are essential in order to
avoid premature discontinuation of the chosen antide-
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54
APA PRACTICE GUIDELINES
pressant medication and to maximize the dose and duration of the antidepressant therapy (40, 218).
Because of pharmacokinetic and pharmacodynamic
differences among individuals, some patients may require
doses higher than those approved by the FDA to achieve
adequate blood levels of a medication and receive therapeutic benefits. Patients who have had their dose increased should be monitored for increased severity of side
effects; dose increases should be considered only for patients who do not have significant or intolerable side effects while taking the medication. Frequent follow-up
contact (either in person or via the phone) may be necessary to address symptoms, side effects, and patient adherence in order to personalize treatment to the specific
clinical needs of the patient. When available and clinically
meaningful, therapeutic ranges for blood levels of antidepressant medications are useful in optimizing medication
dosing (201, 232, 233).
Individual differences are common in the time to response and the tolerability of treatments. For patients who
have shown a partial response to treatment, particularly
those with features of personality disorders and prominent
psychosocial stressors, extending the antidepressant medication trial (e.g., by 4–8 weeks) may allow up to one-third
of patients to respond more fully (417–419).
In patients who are receiving psychotherapy, similar
principles apply in terms of monitoring and adjusting
treatment in the context of nonresponse or difficulty tolerating psychotherapy (331). Factors to be considered include the frequency of sessions, the type of psychotherapy
being used, the quality of the therapeutic alliance, and the
possible need for medications in lieu of or in addition to
psychotherapy. Whereas increasing the frequency of therapy sessions is a reasonable approach to nonresponse, this
approach is based on clinical wisdom and has not been
systematically studied.
b.
Changing to other treatments
Changing to a different non-MAOI antidepressant medication is a common strategy for patients with treatmentresistant major depressive disorder, especially those who
have not shown at least partial response to the initial medication regimen. Although there are no specific patient
characteristics that predict which medication to choose
(420), results from STAR*D suggest that changing to a
second-step treatment results in additional remission rates
of about 25%, and further changes are associated with continued remission, albeit at lower rates (about 13%–14%).
Treatment can be changed to a non-MAOI antidepressant
medication from the same pharmacological class (e.g.,
from one SSRI to another SSRI) or to one from a different
class (e.g., from an SSRI to a TCA) (369, 421–422). Adding
or changing to a depression-focused psychotherapy should
also be considered for patients with major depressive disorder who do not respond fully to medication treatment.
Other strategies for patients who do not respond adequately to pharmacotherapy include changing to an
MAOI after allowing sufficient time between medications
to avoid hazardous interactions (see Table 8). Transcranial
magnetic stimulation could also be an option, as it appears
to be safe and well tolerated (270, 280). In addition, it has
shown small to moderate benefits in most (268, 270–272)
but not all (269, 273) clinical trials and recent meta-analyses. Recent randomized trials suggest that quetiapine
monotherapy also produces a greater reduction in depressive symptoms than placebo (423, 424), with comparable
efficacy to duloxetine (424), although the potential side effects of second-generation antipsychotic treatment need
to be taken into consideration. ECT remains the most effective therapy for patients with treatment-resistant symptoms (239, 425), although results of clinical trials differ
on whether patients with medication-resistant symptoms
have responses to ECT that are comparable to those of
patients without documented medication resistance (426–
428).
c. Augmenting and combining treatments
Pharmacotherapy can be combined with a depressionfocused psychotherapy, both as an initial treatment plan,
and as a strategy to address nonresponse to treatment in
one modality or the other. See Section II.B.4.c above for
further information about combining pharmacotherapy
and psychotherapy.
Antidepressant medications can be augmented with another non-MAOI antidepressant or with other, nonantidepressant agents. The addition of a second non-MAOI
antidepressant may be helpful, particularly for patients
who have had a partial response to antidepressant monotherapy (429). One option is to add a second non-MAOI
antidepressant medication from a different pharmacological class, taking care to avoid drug-drug interactions. Another option is to add an adjunctive, nonantidepressant
medication—such as lithium, thyroid hormone, an anticonvulsant, a psychostimulant, or a second-generation
(atypical) antipsychotic. More information about these
strategies is given later in this section.
Some limited evidence and clinical experience support
the addition of bupropion to an SSRI. This combination
is generally well tolerated, although bupropion, a moderately potent inhibitor of CYP 2D6, increases blood levels
of some SSRIs (430). In one study, combined treatment
with bupropion and an SSRI resulted in better outcomes
than either therapy alone (431). Another commonly used
strategy is the combination of mirtazapine and an SSRI or
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
venlafaxine. Generally, mirtazapine 15–30 mg at bedtime
is added to the incompletely effective antidepressant and
titrated up to 45 mg/day on the basis of response and tolerability (432).
For patients with pronounced anxiety or persistent
insomnia not adequately relieved by an SSRI or SNRI, adjunctive use of anxiolytic and sedative-hypnotic medications is common (433, 434). These include benzodiazepines
such as clonazepam (435) and selective GABA agonists such
as zolpidem (436) and eszopiclone (437). Buspirone has also
been used adjunctively in anxious individuals (429). Although adjunctive therapy of anxiety or insomnia can hasten symptomatic relief, there is no evidence of sustained
benefit, and some patients have difficulty stopping the anxiolytic or hypnotic medication (438, 439).
Lithium, thyroid hormone, and stimulants are sometimes combined with antidepressants to augment response. Lithium is the most extensively studied of these
adjuncts (440–443) and may also reduce the long-term
risk of suicide (444). The interval before full response to
adjunctive lithium is said to be in the range of several days
to 6 weeks. The blood level required to enhance the effects of antidepressants still has not been confirmed. If effective and well tolerated, lithium should be continued at
least for the duration of acute treatment and perhaps beyond the acute phase for purposes of relapse prevention.
Thyroid hormone supplementation, even in euthyroid
patients, may increase the effectiveness of antidepressant
medication treatment, whether used as an augmentation
agent (445, 446) or in combination with an antidepressant
from the outset of therapy (447). The dose typically used
for this purpose is 25 mcg/day of triiodothyronine, increased to 50 mcg/day if the response is inadequate after
about a week. The duration of treatment required has not
been well studied.
Second-generation antipsychotic medications may increase the rates of response or remission of depressive
symptoms in patients who typically have not responded to
more than two medication trials (448), even when psychotic symptoms are not present. Generally, in clinical
practice, lower doses are used for antidepressant augmentation than for treatment of psychosis. For example, the
combination of olanzapine and fluoxetine has been extensively studied (449–452) and is typically initiated with 6 mg
of olanzapine and 25 mg of fluoxetine daily and titrated upward as tolerated to a maximum of 18 mg of olanzapine and
75 mg of fluoxetine daily. Aripiprazole has received FDA
approval for augmentation of antidepressive agents and is
typically initiated at 2.5–5 mg/day and titrated upward as
tolerated to a maximum of 15 mg/day (453). With quetiapine, doses of 25 to 400 mg/day have been used, with benefits for depressive symptoms found in some (454, 455) but
55
not all (456) clinical trials. Risperidone augmentation, in
doses of up to 3 mg daily (457, 458) also appears to improve
the response to antidepressant agents. In most of these trials,
the onset of the effect of second-generation antipsychotic
augmentation has been rapid, although the magnitude of
the advantage relative to placebo has been relatively modest. In the only two trials to utilize active comparison
groups, the combination of olanzapine and fluoxetine was
not significantly more effective at study endpoint than continued therapy with nortriptyline (450) or venlafaxine (451).
Naturalistic follow-up data also suggest that long-term
weight gain can be problematic for many patients receiving
second-generation antipsychotic augmentation therapy,
particularly with the olanzapine-fluoxetine combination
(459). In addition, a recent meta-analysis suggests that the
rate at which SGA augmentation is discontinued is nearly
four-fold greater than study discontinuation among subjects randomly assigned to placebo (448). When compared
with other strategies for antidepressant nonresponders, augmentation with a second-generation antipsychotic carries
disadvantages: the high cost of many agents, the significant
risk of weight gain and other metabolic complications (e.g.,
dyslipidemia, hypertriglyceridemia, glucose dysregulation,
diabetes mellitus), and potential risk of hyperprolactinemia, tardive dyskinesia, neuroleptic malignant syndrome,
and QTc prolongation. Thus, the advantages and disadvantages of antipsychotic medications should be considered
when choosing this augmentation strategy. In addition,
when augmentation with a second-generation antipsychotic
is effective, it is uncertain how long augmentation therapy
should be maintained.
Many clinicians find that augmentation of antidepressants with low doses of stimulants such as methylphenidate
or dextroamphetamine may help ameliorate otherwise
suboptimally responsive depression (460–462), although
not all clinical trials have shown benefits from this strategy (463). More recently, the novel compound modafinil
has shown modest benefit when combined with SSRIs, related to specific effects on residual symptoms such as fatigue and hypersomnolence (464–467). Although there
are no clear guidelines regarding the length of time stimulants or modafinil should be coadministered, in one extension study the effects of modafinil were maintained across
12 weeks of additional therapy (468). Physicians prescribing modafinil for this off-label use should become familiar
with rare but dangerous cutaneous reactions to it, including reported instances of Stevens-Johnson syndrome,
toxic epidermal necrolysis, drug rash with eosinophilia
and systemic symptoms (469), and cytochrome P450 interactions. Modafinil can also induce CYP 3A4 and render
contraceptive medications and other medications metabolized through this route ineffective.
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56
Although their use in this context has not been extensively evaluated, anticonvulsants such as carbamazepine,
valproic acid, and lamotrigine may offer some benefit in
the treatment of medication-resistant major depressive
disorder (121, 429, 470–473).
A rarely used strategy is the combined use of a TCA or
trazodone and an MAOI (474, 475). The combination of a
TCA and an MAOI has been used for more than three
decades for treatment of some of the most treatmentresistant depressive disorders; however, the risk of drugdrug interactions necessitates careful monitoring (119).
Of particular concern with these combinations is the serotonin syndrome, characterized by delirium, hyperthermia,
hyperreflexia, myoclonus, and, rarely, death (see Section
II.B.2.b.5.b). Use of an MAOI in combination with a
TCA and related antidepressants should probably not be
considered until other pharmacological strategies for patients with treatment-resistant illness have been exhausted;
psychiatrists and patients choosing to use the combination of an MAOI and a TCA should be well acquainted
with the potential hazards and carefully weigh the relative
risks and benefits of such a strategy.
Vagus nerve stimulation was approved for use in patients whose symptoms have not responded to at least
four adequate trials of antidepressant medications and/or
ECT. Acute benefits were not observed in the shamcontrolled portion of the VNS trial (282). When compared with a parallel treatment-as-usual arm, the longterm (1–2 year) open-label extension showed small (476,
477) but persistent (478) improvements in symptoms with
VNS that could be clinically significant for some patients.
Other open-label studies have also shown some benefit
when VNS is used simultaneously with pharmacotherapy
(479–481).
As with any surgical device implantation, there is a
small risk of postsurgical infection (482). A majority of individuals experience hoarseness or voice alteration during
stimulation, and coughing, dyspnea, and neck discomfort
are common (281, 481) but generally are tolerable to patients (282, 479). Patients also need to be informed of the
implications of having an implanted VNS device for future medical care (482). For example, with a VNS device
in place, brain MRI requires the use of a special sendreceive coil. The VNS device may affect the operation of
other implanted devices such as cardiac pacemakers or
defibrillators and other procedures such as diathermy, and
whole body or radiofrequency receive-only MRI are contraindicated. VNS is also contraindicated in the presence
of bilateral or left cervical vagotomy.
Relative to other antidepressive treatments, the role of
VNS remains a subject of debate. However, it could be
considered as an option for patients with substantial symp-
APA PRACTICE GUIDELINES
toms that have not responded to repeated trials of antidepressant treatment.
C. CONTINUATION PHASE
Continuation phase pharmacotherapy is strongly recommended following successful acute phase antidepressant
therapy, with a recommended duration of continuation
therapy of approximately 4–9 months (assuming good and
consistent control of depression symptoms). The goal of
continuation treatment is to prevent relapse (i.e., the reemergence of significant depressive symptoms or dysfunction) in the vulnerable period immediately following
remission (i.e., a complete alleviation of symptoms) (408,
410, 411). The possibility of relapse should be carefully
monitored during the continuation phase as this is when
risk of relapse is highest (483). Within the first 6 months
following recovery from a major depressive episode, relapse of depressive symptoms is common, with the proportion of patients with relapse ranging from 20% of patients
in mixed samples (484–487) to as many as 85% of severely
depressed inpatients receiving treatment with ECT (234,
488, 489). These studies also show that relapse rates are
greater if antidepressant treatment (including ECT) is
discontinued or reduced in dose or intensity following recovery (234, 489, 490). There is evidence that patients
who do not completely recover during acute treatment
have a significantly higher risk of relapse (and a greater
need for continuation treatment) than those who have no
residual symptoms (227, 491, 492). Similarly, patients
who have not fully achieved remission with psychotherapy are at greater risk of relapse in the near term (364,
365, 367, 493, 494). To reduce the risk of relapse during
the continuation phase, treatment should generally continue at the same dose, intensity, and frequency that were
effective during the acute phase. Although the number of
randomized controlled trials of antidepressant medications in the continuation phase is limited, the available
data indicate that patients treated for a first episode of uncomplicated major depressive disorder who exhibit a satisfactory response to an antidepressant medication should
continue to receive a full therapeutic dose of that agent for
at least 4–9 months after achieving full remission (105,
225, 495).
Published studies for the continuation phase with older
TCAs as well as newer medications have consistently
shown efficacy of these medications in preventing relapse,
compared with placebo. Lithium has also been shown to
have efficacy in preventing relapse (496).
Cognitive-behavioral therapy may prevent relapse of
depression when used as augmentation to medication
treatment. It may also bestow an enduring, protective ben-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
efit that reduces the risk of relapse after the treatment has
ended (363). Cognitive group therapy helps to prevent relapse and recurrence for patients in remission after a major depressive episode (497). Mindfulness-based cognitive
therapy is a variant of cognitive therapy that encourages
patients to pay attention to their thoughts and feelings in
the moment and to accept them rather than judging or
trying to change or disprove them. Among patients with
remitted depression, mindfulness-based cognitive therapy groups may reduce risk of relapse for patients who
have already experienced three or more episodes (498).
Such benefits for CBT (and potentially, for other psychotherapies) would offer an advantage over pharmacotherapy, which works only as long as the patient continues the
antidepressant medication.
Continuation therapy is also essential in reducing relapse risk after an acute course of ECT (239). Although
relapse occurs for many patients regardless of continuation strategy (234, 488, 489), remission of symptoms following successful treatment with ECT may be maintained
with either pharmacotherapy or continuation ECT (234).
Research shows that continuation ECT is comparable in
efficacy to the combination of nortriptyline and lithium
(234) and that the latter combination is superior to
nortriptyline alone in preventing relapse (489). Although
there is limited information regarding prognostic factors,
relapse may be less likely among patients with melancholic depression who receive continuation ECT after remission with acute ECT than among those who receive
continuation pharmacotherapy after remission with acute
ECT (499).
Given the significant risk of relapse during the continuation phase of treatment, it is essential to assess depressive symptoms, functional status, and quality of life in a
systematic fashion, which can be facilitated by the use of
periodic, standardized measurements. It is often helpful
for patients and families to identify particular signs (e.g.,
lack of engagement in specific activities that are usually enjoyed, specific “signal” symptoms or patterns of thought)
that are typical of their earlier depressive episodes and may
suggest the beginnings of a depressive relapse. Furthermore, any sign of symptom persistence, exacerbation, or
reemergence or of increased psychosocial dysfunction
during the continuation period should be viewed as a harbinger of possible relapse.
If a relapse does occur during the continuation phase, a
return to the acute phase of treatment is required. An initial
step is often to increase the dose of medication (500) or,
with continuation ECT, to increase the frequency of
treatment (501). For patients receiving psychotherapy, an
increased frequency of sessions or a shift in the psychotherapeutic focus may be needed. It is also essential to de-
57
termine whether any specific precipitants are contributing
to the relapse of depression. For example, the onset or
worsening of psychosocial stressors, substance use disorders, or general medical conditions can contribute to increased depressive symptoms. In addition, decreased
treatment adherence or reductions in medication blood
levels (e.g., due to drug-drug interactions or increased cigarette use) can also prompt a depressive relapse.
D. MAINTENANCE PHASE
Patients with chronic and/or recurrent major depressive
disorder who complete the continuation phase without
relapse proceed to the maintenance phase of treatment, in
which the goal is to protect susceptible patients against recurrence of subsequent depression.
Patients who have had three or more prior major depressive episodes should receive maintenance treatment.
Within the first 6 months following recovery from a major depressive episode, 20% of patients will experience a
recurrence (484). Between 50% and 85% of patients will
have at least one lifetime recurrence, usually within 2 or 3
years (502), although there is little consistency in the time
to recurrence for any individual patient (484). Patients
who have had a prior major depressive episode also have a
high risk of experiencing subsequent affective episodes
other than another major depressive episode, such as a
manic, hypomanic, or dysthymic episode (503). The number of lifetime major depressive episodes is significantly
associated with the probability of recurrence, such that the
risk of recurrence increases by 16% with each successive
episode (484).
Maintenance therapy should be considered more
strongly for patients with additional risk factors for recurrence, such as the presence of residual symptoms, ongoing
psychosocial stressors, family history of mood disorders,
and the severity of prior episodes (504) (see Table 10). Additional considerations that may play a role in the decision
to use maintenance therapy include patient preference,
the presence of side effects during continuation therapy,
and the severity of prior depressive episodes, including
factors such as psychosis or suicide risk. Due to the risk of
recurrence and the importance of early detection of recurrent symptoms, patients should be monitored periodically
and in a systematic fashion during the maintenance phase;
such assessments can be facilitated by the use of standardized rating scales, as described in Section II.A.8.
In general, the treatment that was effective in the acute
and continuation phases should be used in the maintenance
phase.
Among the therapeutic options available for maintenance treatment, antidepressant medications have received
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58
TABLE 10.
APA PRACTICE GUIDELINES
Risk Factors for Recurrence of Major Depressive
Disorder
Persistence of subthreshold depressive symptoms
Prior history of multiple episodes of major depressive
disorder
Severity of initial and any subsequent episodes
Earlier age at onset
Presence of an additional nonaffective psychiatric
diagnosis
Presence of a chronic general medical disorder
Family history of psychiatric illness, particularly mood
disorder
Ongoing psychosocial stressors or impairment
Negative cognitive style
Persistent sleep disturbances
the most study. There have been more than 30 trials of pharmacotherapy in the maintenance phase, and results have
generally demonstrated the effectiveness of antidepressant medication for relapse prevention (105, 226, 314, 505–
507). Many of these trials used TCAs (314, 506), although
results of trials involving newer antidepressant medications have been assessed in a recent meta-analysis (507).
Lithium has also been used as maintenance treatment for
major depressive disorder (441). Despite this, there is limited information on many of the clinical decisions involving
medication use in the maintenance phase. Even though
lower doses of medication are less likely to produce side
effects, results from one study suggest that full doses are
superior to lower doses in the maintenance phase (508).
Particularly if medications are well-tolerated, it is generally advisable to prescribe the same antidepressant medication doses for maintenance therapy that were effective
in prior phases of treatment. Even with adequate maintenance treatment, pharmacotherapy is not invariably successful in preventing relapse and return of symptoms, which
still occur in as many as 25% of individuals (509, 510). It is
unclear whether some relapses during maintenance therapy are loss of therapeutic efficacy, a phenomenon that
has been referred to as tachyphylaxis, but many such relapses appear related to inadequate prophylactic effects
of medication (511). When relapses occur, clinicians
typically address them using the same approaches described
to treat incomplete responses to treatment, such as increasing the dose of medication, changing to a different
medication, or adding another medication or a depressionfocused psychotherapy to augment therapeutic response
(510, 512).
There have been fewer investigations of the effectiveness of psychotherapy in the maintenance phase. Nonethe-
less, several studies have shown that acute psychotherapies
for major depressive disorder also have maintenance benefits. For example, even once-monthly maintenance IPT
has been shown to forestall relapse in patients at high risk
for relapse (289, 314, 315, 513). Most of these studies have
used once-monthly maintenance IPT, but research has
not demonstrated that frequency of sessions affects outcome (289). In one study, maintenance cognitive therapy
delivered over 2 years was as effective as maintenance
medication for recurrent major depressive disorder (514).
Combining psychotherapy—such as CBT, cognitive therapy, or IPT—with pharmacotherapy in the maintenance
phase has also been considered by investigators. Some
results suggest that the combination of antidepressant
medications plus psychotherapy may be more effective in
preventing relapse than treatment with single modalities
(314, 365, 506, 515, 516).
For patients receiving treatment with pharmacotherapy and/or psychotherapy, the frequency of visits during
the maintenance phase should be set according to the
clinical condition and the specific treatments being used.
The frequency can range from as low as once every several
months for stable patients who require only psychiatric
management and medication monitoring to as high as
once or twice per week for those receiving psychodynamic
psychotherapy. For CBT and IPT, maintenance-phase
treatments usually involve a decreased frequency of visits
(e.g., once a month). The duration of the maintenance
phase will vary depending on the frequency and severity
of prior major depressive episodes, the tolerability of
treatments, and patient preferences. For many patients,
some form of maintenance treatment may be required indefinitely.
Electroconvulsive therapy has also been used in the
maintenance phase, although evidence for its benefits
comes largely from case reports (239). Patients who exhibit
repeated episodes of moderate or severe major depressive
disorder despite optimal pharmacological treatment or patients who are medically ineligible for such treatment may
be maintained with periodic ECT. Although the optimal
frequency and duration of maintenance phase ECT treatments has not been well studied, maintenance ECT is
often administered monthly; individuals for whom this
is insufficient may find treatment at more frequent intervals to be beneficial (501).
E. DISCONTINUATION OF TREATMENT
If maintenance-phase treatment is not indicated, stable
patients may be considered for discontinuation of treatment after the continuation phase. The precise timing
and method of discontinuing psychotherapy and pharma-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
cotherapy for major depressive disorder have not been
systematically studied.
The decision to discontinue treatment should be based
on the same factors considered in the decision to initiate
maintenance treatment (Table 10), including the probability of recurrence, the frequency and severity of past episodes, the persistence of depressive symptoms after
recovery, the presence of co-occurring disorders, and patient preferences. The type of treatment being received
may also play a role in the decision making. In general,
psychotherapy has a longer lasting treatment effect and
carries a lower risk of relapse following discontinuation
than pharmacotherapy. In terms of timing, patients should
be advised not to discontinue medications before holidays,
significant events (e.g., weddings), or stressful events.
Patients should be carefully monitored during and immediately after treatment discontinuation to ensure that
remission is stable. The highest risk for a relapse is seen in
the first 2 months after discontinuation of treatment.
Hence, it is important to schedule a follow-up visit during
this period to ensure stability.
When pharmacotherapy is being discontinued, it is
best to taper the medication over the course of at least
several weeks. Such tapering allows for the detection of
recurring symptoms at a time when patients are still partially treated and therefore more easily returned to full
therapeutic treatment if needed. In addition, such tapering can help minimize the incidence of antidepressant
medication discontinuation syndromes, particularly with
paroxetine and venlafaxine (98, 163, 164). Discontinuation
syndromes are problematic because their symptoms include disturbances of mood, energy, sleep, and appetite
and can therefore be mistaken for or mask signs of relapse
(517). Consequently, patients should be advised not to
stop medications abruptly and to take medications with
them when they travel or are away from home. Discontinuation syndromes have been found to be more frequent after discontinuation of medications with shorter half-lives,
and patients maintained on short-acting agents should
III.
59
have their medications tapered gradually over a longer period (518, 519). Another strategy is to change to a brief
course of fluoxetine, e.g., 10 mg for 1–2 weeks, and then
discontinue the fluoxetine (165). The psychiatrist should
closely monitor patients withdrawing from antidepressants and provide reassurance that symptoms are timelimited and can be addressed by more gradual tapering
(see Section II.B.2.b.1.i).
How to end psychotherapy is typically dependent on
the type of therapy. For time-limited approaches, termination is usually broached from the initiation of treatment
and periodically revisited, as the therapist-patient dyad
notes which session they are in, how many remain, and
how they have progressed toward defined goals. In dynamically oriented psychotherapy, the therapist typically
raises termination as an issue well in advance of the final
session, using the opportunity to explore remaining and
unresolved issues in transference.
Before the discontinuation of active treatment, patients should be informed of the potential for a depressive
relapse. Early signs of major depressive disorder should be
reviewed, often with a family member, and a plan established for seeking treatment in the event of recurrent
symptoms. Patients should continue to be monitored
over the next several months to identify early evidence of
recurrent symptoms. Again, systematic assessment of
symptoms, side effects, adherence, and functional status
during this period of high vulnerability is strongly recommended. If a patient does suffer a recurrence after discontinuing medication, treatment should be promptly
reinitiated. Usually, the previous treatment regimen to
which the patient responded in the acute and continuation
phases should be reinitiated (520). Patients who have a recurrence following discontinuation of antidepressant
therapy should be considered to have experienced another
major depressive disorder episode and should receive
adequate acute-phase treatment followed by continuation-phase treatment and possibly maintenance-phase
treatment.
SPECIFIC CLINICAL FEATURES INFLUENCING THE
TREATMENT PLAN
A. PSYCHIATRIC FACTORS
1. Depressive symptoms
a. Suicidal ideation and behaviors
Because suicide is the worst outcome of major depressive
disorder, a patient’s risk for suicide must be assessed re-
peatedly over the course of treatment. For patients who
report suicidal ideation, intention, or planning, close surveillance is necessary (see Sections II.A.3 and II.A.4). Psychiatrists should consider greater intensity of treatment
for suicidal patients, including hospitalization when warranted and/or combined treatment with pharmacother-
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60
apy and psychotherapy. In patients at high risk for suicide
and in whom a particularly rapid antidepressant response
is required, consideration should be given to the use of
ECT (239, 243, 521). Patients with major depressive disorder who present to an emergency department with suicidal ideation, or who have made a suicide attempt, should
be triaged to determine their level of safety and establish
the appropriate level and setting of care. Upon entrance
to the emergency department, they should be searched to
permit removal of potentially dangerous items, such as
weapons and personal belongings that could cause harm
(e.g., sharp objects, belts, shoes, medications). Factors to
consider in determining the nature and intensity of treatment include (but are not limited to) access to and lethality of suicide means, past and family history of suicidal
behavior, co-occurring substance abuse, the availability
and adequacy of social supports, and the nature of the
doctor-patient alliance.
To lower the risk of suicide, the psychiatrist should also
treat modifiable risk factors, such as anxiety (especially
panic attacks), insomnia, agitation, psychotic symptoms,
and substance abuse (22), in addition to treating the major
depressive episode. Among inpatients who died by suicide,
Busch et al. (522) observed that a great majority were
admitted for indications other than suicidal ideation, and
anxiety and agitation were common, suggesting that such
symptoms should be addressed if they are present. Family
members can also play an important role in detecting and
preventing suicidal behaviors. When permitted by the patient, the psychiatrist should educate those close to the
patient concerning appropriate interventions and encourage communication.
There has been a growing controversy about the risk of
suicidal ideas and behaviors (sometimes referred to as
“suicidality”) after initiation of antidepressant treatment.
Although information on such risk continues to evolve, a
predictive relationship to suicide has never been demonstrated. Clinical experience has long suggested that patients may develop the energy and capacity to act on selfdestructive plans made earlier in the course of their illness
if neurovegetative and psychomotor symptoms respond
to antidepressant treatment before mood improves. More
recently, meta-analyses of data from clinical trials have
shown statistically significant increases in suicidal thoughts
or behaviors in individuals age 25 years or younger who
are treated with antidepressant medication, compared
with placebo, with an approximately 1.5- to 2.5-fold increase in the relative risk (26, 523–530). In percentage
terms, it is estimated that one to three of 100 individuals
age 25 years or younger could potentially have an increase
in suicidal thoughts or behaviors with antidepressant
treatment (26), although there has been no evidence of in-
APA PRACTICE GUIDELINES
creased mortality in the study subjects as a result of suicide
(531). To alert clinicians to the need for vigilance and
communication during the initial phase of antidepressant
treatment, the FDA has issued a black-box warning pertaining to children, adolescents, and young adults that advises of this increase in the risk of suicidal thinking and
behavior; information on the warning is available on the
FDA Web site at http://www.fda.gov/cder/drug/antidepressants/default.htm. In making decisions about treatment, this awareness of a potential increase in suicidal
thinking and behavior in children, adolescents, and young
adults must be balanced against the negative effects, including suicide, of untreated depression (532) as well as
the demonstrated benefits of antidepressant treatment
(523, 533–535). For adults age 65 years or older, a review
of the evidence from clinical trials showed a decrease in
the risk of suicidal thinking or behaviors with antidepressant treatment, with no change in risk detected for other
adults (age 25 to 64 years) (536).
For additional details about the treatment of suicidal
individuals, clinicians are encouraged to consult APA’s
Practice Guideline for the Assessment and Treatment of Patients With Suicidal Behaviors (22).
b. Major depressive disorder–related cognitive dysfunction
Cognitive inefficiency and impairment are common features of major depressive disorder. Many depressed patients
report slowed thoughts, poor concentration, distractibility,
and reduced capacity to process information. They also display diminished attention to self-care and to their environment. Transient cognitive impairment, especially involving
attention, concentration, and memory storage and retrieval,
are demonstrable through neuropsychological testing (537).
In extreme cases, especially in elderly patients, these deficits
are so prominent that patients appear to have dementia. For
individuals who exhibit symptoms of a dementia syndrome,
it is crucial that any underlying depressive disorder be identified and treated.
Among depressed patients, the differential diagnosis of
cognitive dysfunction includes degenerative dementias
(such as Alzheimer’s disease and Pick’s disease) and reversible causes (such as vitamin B12 deficiency, folate deficiency,
testosterone deficiency, substance use). Several clinical features help distinguish major depressive disorder–related
cognitive dysfunction from other dementia syndromes.
When performing cognitive tasks, depressed patients generally exert less effort and report greater incapacity than do
patients with dementia. The latter, especially in more advanced stages, typically do not recognize their cognitive
failures, since insight is impaired. In contrast, depressed
patients may report being unable to think or remember.
Patients with major depressive disorder–related cognitive
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
dysfunction lack the signs of cortical dysfunction (i.e., aphasia, apraxia, agnosia) encountered in dementias such as
Alzheimer’s disease (538, 539). Nevertheless, distinguishing
dementia from depression-related cognitive dysfunction
can be difficult, particularly as the two may coexist. For further discussion of the co-occurrence of dementia and depression, the reader may also wish to consult APA’s Practice
Guideline for the Treatment of Patients With Alzheimer’s Disease and Other Dementias, Second Edition (539).
The detection of major depressive disorder–related
cognitive dysfunction alerts the psychiatrist to the need
for treatment of the underlying major depressive disorder,
which should in turn reduce the signs and symptoms of
the cognitive dysfunction. Although initially reversible,
major depressive disorder–related cognitive dysfunction
increasingly appears to be a harbinger of subsequent dementia (540, 541). In addition, research suggests that certain types of executive cognitive dysfunction predict greater
disability and limited treatment response in geriatric patients with depression (542, 543).
2. DSM depressive subtypes
a.
Psychotic features
Major depressive disorder is sometimes accompanied by
hallucinations or delusions, which may be congruent or
incongruent with the depressed mood. Recognition of
psychosis is essential among patients with major depressive disorder as it is often undetected, resulting in ineffective treatment (544–546). Psychotic features constitute a
risk factor for recurrent major depressive disorder and recurrent psychosis and hence indicate the need for maintenance treatment.
Electroconvulsive therapy is highly effective in treating
psychotic depression (241) and can be considered as a
first-line treatment option whenever major depressive
disorder is associated with psychotic features (239, 243,
547). Pharmacotherapy can also be used as a first-line
treatment option for major depressive disorder with psychotic features. Psychotic depression typically responds
better to the combination of an antipsychotic and an antidepressant medication rather than treatment with either
component alone (547–549), although some research has
shown comparable responses for antidepressive treatment
or antipsychotic treatment alone (550, 551). Lithium augmentation is helpful for some patients who have not responded to combined treatment with antidepressant and
antipsychotic medication (262, 552).
b. Catatonic features
A catatonic syndrome sometimes occurs in the context of
major depressive disorder (553–556) and is characterized
61
by at least two of the following manifestations: immobility, as evidenced by catalepsy or stupor; extreme agitation;
extreme negativism; peculiarities of voluntary movement,
as evidenced by posturing, stereotyped movements, mannerisms, or grimacing; and echolalia or echopraxia (556,
557). The presence of catatonia should prompt a thorough differential diagnosis as it can also occur in association with general medical conditions and with several
other psychiatric disorders, including bipolar disorder
and schizophrenia (556, 558, 559). Catatonic signs often
dominate the clinical presentation and may be so severe as
to be life-threatening, compelling the consideration of urgent somatic treatment. Patients with catatonic features
may also need supportive medical interventions including
hydration, nutrition, prophylaxis against deep vein thrombosis, turning to prevent bed sores, and passive range of
motion to prevent contractures. Intravenous administration of a benzodiazepine (e.g., lorazepam, diazepam) or a
barbiturate (e.g., amobarbital) may induce rapid relief
(242, 553) and can be followed by continued oral administration for patients who show an initial response. When
such intervention is ineffective, the clinician should consider the urgent use of ECT (239, 242). The efficacy of
ECT in catatonia is well documented in the case series
literature (239) and is usually apparent after a few treatments. After catatonic manifestations recede, antidepressant medication treatments may be needed during acute
and maintenance phases of treatment. In addition to antidepressant medications, ongoing treatment may include
ECT, lithium, antipsychotics, or a combination of these
approaches, depending upon the patient’s condition. Patients with catatonia may have an increased susceptibility
to neuroleptic malignant syndrome when exposed to antipsychotic medications (560), and this should be considered in planning treatment.
c. Melancholic features
Melancholic features describe characteristic somatic
symptoms, such as the loss of interest or pleasure in all, or
almost all, activities or a lack of reactivity to usually pleasurable stimuli. Other symptoms include worsened depression in the morning, early morning awakening, and
significant anorexia or weight loss, among others (16).
Major depressive disorder with melancholic features is responsive to both pharmacotherapy and ECT. Serotonin
norepinephrine reuptake inhibitors and TCAs may have
an advantage over SSRIs for this patient population (561,
562). Psychotherapy may be less appropriate for patients
with melancholia (563), particularly if the symptoms prevent engagement with the therapist (e.g., lack of interest
in activities). Major depressive disorder with melancholic
features may also be associated with an added risk of sui-
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62
cide (564) and an increased risk of subsequent recurrence
despite the use of maintenance pharmacotherapy (509).
d. Atypical features
Major depressive disorder with atypical features is characterized by a pattern of marked mood reactivity and at least
two additional symptoms, including leaden paralysis, a
long-standing pattern of interpersonal rejection sensitivity,
significant weight gain or increase in appetite, and hypersomnia (the latter two of which are considered reversed
vegetative symptoms) (16). The phrase “atypical features”
distinguishes this depressive subtype from the more classical “endogenous” presentation of depression, but it does
not connote an uncommon or unusual form of depression.
Atypical features are more common in women, are associated with an earlier age at onset of depression and a greater
degree of associated anxiety disorders, and frequently have
a more chronic, less episodic course, with only partial interepisode recovery (565, 566). These atypical features are
also common in the depressed phase of bipolar I disorder
and bipolar II disorder (567, 568), indicating a need for
careful screening for manic or hypomanic episodes in patients who present with atypical depressive symptoms.
In the treatment of major depressive disorder with
atypical features, MAOIs have greater efficacy than TCAs
(122, 569–572). Some data also support the use of SSRIs,
bupropion, and CBT in this patient population (573–
577). Electroconvulsive therapy is also effective in treating patients with atypical features (578). The presence and
severity of specific symptoms as well as safety considerations should help guide the choice of treatment for major
depressive disorder with atypical features. For example, if
a patient does not wish to, cannot, or appears unlikely to
adhere to the dietary and medication precautions associated with MAOI treatment, the clinician should consider
alternative antidepressant medication or psychotherapy.
e. Seasonal pattern
A seasonal pattern of major depressive disorder is characterized by a regular temporal relationship between particular periods of the year and the onset and remission of
symptoms, which is not the result of seasonally related
psychosocial stressors (e.g., seasonal unemployment, significant anniversaries). The most common presentation
in the northern hemisphere is the regular appearance of
symptoms between early October and late November and
regular remission from mid-February to mid-April. Episodes of major depressive disorder with seasonal pattern
frequently have atypical features such as hypersomnia and
overeating. Some of these patients experience manic or
hypomanic episodes as well; hence, it is important to diagnose bipolar disorder when appropriate.
APA PRACTICE GUIDELINES
The entire range of treatments for major depressive
disorder may be used to treat major depressive disorder
with seasonal pattern, either in combination with or as an
alternative to light therapy. As a primary treatment, light
therapy may be recommended as a 1- to 2-week time-limited
trial (395), primarily for outpatients with clear seasonal
patterns. For patients with more severe forms of major
depressive disorder with seasonal pattern, the use of light
therapy is considered adjunctive to pharmacological intervention. In terms of specific antidepressive agents, the
extended release formulation of bupropion is FDA approved
for use with patients who have major depressive disorder
with seasonal pattern.
3. Co-occurring psychiatric disorders
Co-occurring psychiatric disorders generally complicate
treatment. Patients with major depressive disorder who
also have other psychiatric disorders have greater symptom severity and are more challenging to treat than patients with major depressive disorder alone. Yet the
presence of co-occurring Axis I or Axis II disorders should
not lead clinicians to conclude that patients are untreatable. Furthermore, other Axis I or Axis II disorders may
masquerade as major depressive disorder or may seem to
co-occur with the depression. In these cases, the other apparent disorders evanesce with successful treatment of the
underlying major depressive disorder.
a.
Dysthymic disorder
Dysthymic disorder is a chronic mood disorder with
symptoms that fall below the threshold for major depressive disorder. Because of this, it may escape notice and
may be inadequately treated. Nonetheless, it can cause
significant suffering and disability. In some patients, both
dysthymic disorder and major depressive disorder (socalled “double depression”) may be diagnosed.
In the treatment of dysthymic disorder and chronic
major depressive disorder, there is demonstrated efficacy
for antidepressant medications, including TCAs, SSRIs,
other newer agents, and MAOIs. Unfortunately, clinical
trials provide little evidence of the relative efficacies of
particular agents (105, 579). In general, pharmacotherapy
of dysthymic disorder resembles that for episodes of
major depressive disorder; responses to antidepressant
medications by patients with dysthymic and chronic
major depressive disorders have been comparable to the
responses by patients with major depressive disorder
episodes (580). In “double depression,” antidepressant
medication can reverse not only the acute major depressive episode but also the co-occurring dysthymic disorder
(581).
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
Patients with dysthymic disorder, as well as patients
with chronic and severe major depressive disorder, typically have a better response to the combination of pharmacotherapy and psychotherapy than to either alone
(294, 295), although results of combined treatment studies have been mixed and complicated by methodological
problems (582).
b. Anxiety disorders
As a group, anxiety disorders are the most commonly occurring psychiatric disorders in patients with major depressive disorder (583). A 2005 epidemiological study
found that among individuals with major depressive disorder, 62% also met the criteria for generalized anxiety
disorder, 52% for social phobia, 50% for posttraumatic
stress disorder (PTSD), 48% for panic disorder, 43% for
specific phobia, and 42% for obsessive-compulsive disorder (584). In addition, agitation and anxiety, including
panic attacks, are frequent co-occurring symptoms of
major depressive disorder. The appearance of anxiety and
agitation in patients in a major depressive episode, particularly when accompanied by racing or ruminative thoughts,
should alert the clinician to the possibility of a mixed
mood state of a bipolar spectrum disorder (585).
In studies of major depressive disorder with a cooccurring anxiety disorder, both depressive symptoms and
anxiety symptoms respond to antidepressant medication
treatment (586). However, TCAs and SSRIs may initially
worsen rather than alleviate anxiety symptoms, including
panic attacks; patients should be so advised, and these
medications should be introduced at low doses and slowly
increased when treating such patients. Adjunctive antipanic agents, such as benzodiazepines, may be necessary
as well. Selective serotonin reuptake inhibitors are beneficial for patients with co-occurring depression and social
anxiety disorder (587) and co-occurring depression and
PTSD (588). Bupropion is comparable to SSRIs in the
treatment of patients with major depressive disorder and
low to moderate levels of anxiety (82), but studies vary as
to whether bupropion is (589) or is not (590) effective in
the treatment of panic disorder. Because benzodiazepines
are not antidepressants and carry their own adverse effects
and toxicity, including abuse and dependence, benzodiazepines should not be the primary pharmacological agents
for patients with major depressive disorder who have cooccurring anxiety symptoms. These agents may be used
adjunctively with other antidepressive treatments, however (591). Psychotherapies such as CBT, behavioral therapy, and IPT may also be used to treat anxiety symptoms
in the context of major depressive disorder (591, 592).
Obsessive-compulsive symptoms are also common in
patients with major depressive episodes. In addition, ob-
63
sessive-compulsive disorder may appear as a co-occurring
condition in some patients with major depressive disorder. Clomipramine and SSRIs have demonstrated efficacy
in managing obsessive-compulsive symptoms in addition
to treating depression (593–595).
c. Dementia
Patients with dementia are predisposed to depression, and
the psychiatrist should therefore screen for depression in
this population, although this is sometimes challenging
(539). One screening tool is the Cornell Scale for Depression in Dementia, which incorporates self-report with
caregiver and clinician ratings of depressive symptoms
(596). Treatment of major depressive disorder in the cognitively impaired patient requires careful supervision and
monitoring of the patient’s pharmacotherapy; this may
entail education of home health aides, nursing home staff,
and others. Antidepressants are likely to be efficacious in
treatment of depressive symptoms, but they do not improve cognition, and data on antidepressant use in patients with dementia are limited (597–599). Individuals
with dementia are particularly susceptible to the adverse
effects of muscarinic blockade on memory and attention.
Therefore, individuals with dementia generally do best
when given antidepressant medications with the lowest
possible degree of anticholinergic effect, e.g., bupropion,
fluoxetine, sertraline, trazodone, and, of the tricyclic
agents, desipramine or nortriptyline (600). Alternatively,
some patients do well when given stimulants in small
doses. Electroconvulsive therapy is also effective in major
depressive disorder superimposed on dementia. It should
be used if medications are associated with an excessive risk
of adverse effects, are not tolerated, or if immediate resolution of the major depressive disorder episode is medically indicated (such as when it interferes with the
patient’s acceptance of food). In individuals with dementia, ECT treatment may be associated with a transient
worsening of the patient’s cognitive status (239, 601, 602).
APA’s Practice Guideline for the Treatment of Patients With
Alzheimer’s Disease and Other Dementias, Second Edition
(539) contains more information about the treatment of
depression and dementia.
d. Substance use disorders
Major depressive disorder frequently occurs with alcohol
or other substance abuse or dependence. Therefore, the
psychiatrist should obtain a detailed history of the patient’s substance use. With the patient’s permission, family
members, friends, or co-workers can be collateral sources
of information. If the evaluation reveals a substance use
disorder, this should be addressed in treatment. A patient
with major depressive disorder who has a co-occurring
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64
APA PRACTICE GUIDELINES
substance use disorder is more likely to require hospitalization, more likely to attempt suicide, and less likely to
adhere to treatment than a patient with major depressive
disorder of similar severity uncomplicated by substance
use (603–608).
Detoxifying patients before initiating antidepressant
medication therapy is advisable when possible (110). Antidepressants may be used to treat depressive symptoms
following initiation of abstinence if symptoms do not improve over time. It is difficult to identify patients who should
begin a regimen of antidepressant medication therapy
soon after initiation of abstinence, because depressive
symptoms may have been induced by intoxication and/or
withdrawal of the substance. A family history of major depressive disorder, a history of major depressive disorder
preceding alcohol or other substance abuse, or a history of
major depressive disorder during periods of sobriety raises
the likelihood that the patient might benefit from antidepressant medication, which may then be started early in
treatment. Comparing the temporal pattern of symptoms
with the periods of use and abstinence of the substance
may help to clarify the patient’s diagnosis. Repeated, longitudinal psychiatric assessments may be necessary to distinguish substance-induced depressive disorder from cooccurring major depressive disorder, particularly because
some individuals with substance use disorders reduce
their substance consumption once they achieve remission
of a co-occurring major depressive disorder.
Co-occurring substance use, especially with stimulant
drugs, raises the risk of deleterious interactions with MAOIs,
although few such events have been reported (609). Benzodiazepines and other sedative-hypnotics carry the potential for abuse or dependence and should rarely be
prescribed to patients with co-occurring substance use
disorders, except as part of a brief detoxification regimen.
Hepatic dysfunction and hepatic enzyme induction frequently complicate pharmacotherapy of patients with alcoholism and other substance abuse. These conditions
may require careful monitoring of blood levels (as appropriate for the medication), therapeutic effects, and side effects to avoid the opposing risks of either psychotropic
medication intoxication or underdosing.
For individuals with nicotine dependence who wish to
stop smoking, bupropion and nortriptyline treatment increase smoking cessation rates by about twofold (109) and
would be useful to consider when selecting a specific antidepressive agent (110).
e.
Personality disorders
For patients who exhibit symptoms of both major depressive disorder and a personality disorder, psychiatrists
should consider appropriate treatment for each. Major
depressive disorder should generally be the initial target;
if evidence of a personality disorder persists when the depressive symptoms have resolved, psychotherapeutic and
adjunctive pharmacotherapeutic approaches may be helpful (610–615). Patients with virtually any personality disorder exhibit a less satisfactory antidepressant medication
treatment response, in terms of both social functioning
and residual major depressive disorder symptoms, than do
individuals without personality disorders (616). Personality disorders tend to interfere with treatment adherence
and development of a psychotherapeutic relationship. Furthermore, many personality disorders increase the risk of
episodes and increase time to remission of major depressive disorder (617, 618). Patients with various personality
disorders also showed high rates of new-onset major depressive episodes in a large prospective study (619) and were
at higher risk of attempting suicide than patients without
a co-occurring personality disorder (620).
Axis II diagnoses should be made with caution during a
major depressive episode, as depressive symptoms may exaggerate or mimic personality traits. Treatment of the depressive disorder for these patients can cause the apparent
personality disorder symptoms to remit or greatly diminish. Depressed patients may believe that their current
symptoms have been present from early life, when in fact
they only began with the current episode. Such misperceptions often hinder accurate diagnosis. Some Cluster C
personality disorders (e.g., avoidant, dependent, obsessive-compulsive) may reflect the residual impact of recurrent
depressive symptoms and may remit with maintenance
therapy (621).
Patients with borderline personality disorder have a
particularly high rate of major depressive disorder: 20%
in a community sample (622) and 50% in clinical samples
(623). About 10%–15% of patients with major depressive
disorder have co-occurring borderline personality disorder (624), and the percentage increases significantly in
hospital and partial hospital samples. Patients with borderline personality disorder often exhibit mood lability,
rejection sensitivity, inappropriate intense anger, and depressive “mood crashes.” These symptoms are also common in patients with depression, particularly with atypical
features, complicating the diagnosis of these disorders.
Antidepressants are in general less effective in treating depressive episodes in patients with major depressive disorder and borderline personality disorder (625–629), with
an overall response rate to all therapies of 20% (630).
For patients with major depressive disorder and borderline personality disorder, the personality disorder must
also be addressed in treatment. Symptoms of both disorders can initially be treated with an SSRI or SNRI. Behavioral impulsivity and dyscontrol can also be treated
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
with low-dose antipsychotics, lithium, and some antiepileptic medications. Monoamine oxidase inhibitors, although efficacious, are not recommended due to the risk of
serious side effects and the difficulties with adherence to
dietary restrictions. Psychotherapeutic approaches such as
dialectical behavioral therapy and psychodynamic psychotherapy have been useful in treatment of borderline
personality disorder as well. In patients with borderline
personality disorder particular attention must be paid to
the maintenance of therapeutic rapport, which is frequently
disrupted, and to the risk of self-harm and suicide, which
occurs in 8%–10% of such individuals. More information
about the treatment of borderline personality disorder can
be found in APA’s Practice Guideline for Treatment of Patients
With Borderline Personality Disorder (610).
f. Eating disorders
Eating disorders are also common in patients with major
depressive disorder (631). Selective serotonin reuptake
inhibitors are the best studied medications for treatment
of eating disorders, with fluoxetine having the most evidence for the effective treatment of bulimia nervosa (170).
Antidepressants may be less effective in patients who are
severely underweight or malnourished, and normalizing
weight should take priority in these patients. Although
SSRIs and psychotherapy are widely used for patients
with anorexia nervosa, the evidence base on which these
practices rest is modest. Patients with chronic anorexia
nervosa have in general been less responsive to formal
psychotherapy. On the other hand, evidence strongly supports the use of CBT in the treatment of bulimia nervosa.
Other therapies (e.g., IPT, group therapies, family therapy) and medications such as SSRIs have also been studied
and have demonstrated effectiveness for this disorder.
Bupropion should be avoided in individuals with eating
disorders due to the increased risk of seizures in these patients. Electroconvulsive therapy has not generally been
useful in treating eating disorder symptoms. Although
there are few data to guide treatment of co-occurring major depressive disorder and eating disorders, it is reasonable to optimize treatment of both disorders based on
these and other considerations. More information about
the treatment of eating disorders can be found in APA’s
Practice Guideline for the Treatment of Patients With Eating
Disorders, Third Edition (170).
B. DEMOGRAPHIC AND PSYCHOSOCIAL
VARIABLES
1. Major psychosocial stressors
Major depressive disorder may follow a substantial adverse life event, especially one that involves the loss of an
65
important relationship or life role. This is particularly
true in initial episodes of depression, with psychosocial
stressors being less associated with the onset of recurrent
episodes (632). Lower socioeconomic status, nonmarried
status, unemployment, urbanization, and violent trauma
seem to increase the risk of developing major depressive
disorder, whereas religious belief may decrease it (633–
635). Among those exposed to trauma, the prevalence of
major depressive disorder seems to be higher among persons who develop PTSD than among those who do not
(636). A recent meta-analysis underlined that among refugees, PTSD was diagnosed in one of 10 and one in 20 had
major depressive disorder (637).
Marital discord has been identified as a potent risk factor
in women for the development of depression (638, 639).
Problems in the family setting may become an ongoing
stressor that hampers the patient’s response to treatment.
Ambivalent, abusive, rejecting, or highly dependent family
relationships may predispose an individual to major depressive disorder. The psychiatrist should screen for such factors and consider family therapy, as indicated, for these
patients. Family therapy may be conducted in conjunction
with individual and pharmacological therapies. Even for instances in which there is no apparent family dysfunction, it
is important to provide the family with education about the
nature of the illness and to enlist the family’s support and
cooperation with the treatment.
The psychiatrist may choose to treat a major depressive
episode with an antidepressant, even if a major stressor
preceded the episode. Nonetheless, attention to the relationship of both prior and concurrent life events to the
onset, exacerbation, or maintenance of major depressive
disorder symptoms is an important aspect of the overall
treatment approach and may enhance the therapeutic alliance, help to prevent relapse, and guide the current
treatment. A close relationship between a life stressor and
major depressive disorder suggests the potential utility of
a psychotherapeutic intervention coupled, as indicated,
with somatic treatment.
2. Bereavement
Bereavement is a particularly severe stressor that can trigger a major depressive episode. However, grief, the natural
response to bereavement, resembles depression, and this
sometimes causes confusion. Psychiatrists treating bereaved individuals should differentiate symptoms of normal
acute grief, complicated grief, and major depressive disorder, as each of these disorders requires a unique management plan. Normal grief should be treated with support
and psychoeducation about symptoms and the course of
mourning; complicated grief requires a targeted psychotherapy, with or without concomitant medication (535,
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66
640); and major depressive disorder should be treated with
medication and/or depression-focused psychotherapy.
Acute grief is the universal reaction to loss of a loved
one, and it is a highly dysphoric and disruptive state (641).
Acute grief is characterized by prominent yearning and
longing for the person who died, recurrent pangs of sadness and other painful emotions, preoccupation with
thoughts and memories of the person who died, and relative lack of interest in other activities and people. Despite
the similarity with depression, only about 20% of bereaved people meet the criteria for major depressive disorder. Successful mourning leads to resolution of acute
grief over a period of about 6 months. Integrated grief remains as a permanent state in which there is ongoing sadness about the loss often accompanied by ongoing feelings
of yearning for the person who died. However, when the
death is accepted, and grief integrated, the person is again
interested in his or her own life and other people.
Complicated grief is a recently recognized syndrome in
which symptoms of acute grief are prolonged, associated
with intense and persistent yearning and longing for the
deceased person, and complicated by guilty or angry ruminations related to the death and/or avoidance behavior.
Studies of individuals bereaved by the attacks of September, 11, 2001, have demonstrated that complicated grief is
a distinct condition from either major depressive disorder
or PTSD (642, 643). It is important to note that treatment
for depression is not effective in relieving symptoms of
complicated grief (640).
Although DSM-IV-TR excludes the diagnosis of major
depressive disorder during the first 2 months following
bereavement, major depressive disorder in the wake of bereavement can impede the course of mourning. Bereavement-related depression responds to antidepressant
medication and should be treated; otherwise it is likely to
become chronic and impairing (644). There is no indication that depression in the context of bereavement differs
from other major depressive episodes, and data indicate
that chronicity of bereavement-related depression over
13 months is similar to chronicity of depression in other
contexts (644).
3. Culture and ethnicity
An appreciation of cultural and ethnic variables is important to the accurate diagnosis of major depressive disorder
and in the selection and conduct of psychotherapy and
pharmacotherapy (645–647). Although major depressive
disorder is seen across cultural and ethnic groups, and the
age at onset, gender differences, and prevalence of co-occurring conditions are similar across cultures, the actual
incidence and prevalence of depression vary (648–656).
Furthermore, some evidence suggests that patients of dif-
APA PRACTICE GUIDELINES
ferent cultures express depressive symptoms differently,
particularly somatic and psychomotor symptoms (657).
Specific cultural variables may also influence the assessment of major depressive disorder symptoms. For example, in some cultures, depressive symptoms may be more
likely to be attributed to physical diseases (658). In addition, language barriers can impede accurate psychiatric
diagnosis and effective treatment (659), and, even when
speaking the same language, individuals of different cultures may use different psychological terms to describe
their symptoms (6, 7). In addition, the importance of individual experience should not be underestimated in the
therapeutic relationship (660). The assessment and treatment process can also be influenced by religious beliefs
(5). Individuals with high levels of religious involvement
may have diminished rates of major depressive disorder
(661, 662).
Differences in the utilization of psychiatric services by
some cultural and ethnic groups have been well documented. Relative to Caucasians, African Americans and
Latinos appear less likely to receive treatment for mood
disorders (663–665).
Several studies have underscored the lower frequency
of use of antidepressant drugs (and more specifically,
SSRIs) (648, 666–669), ECT (670), and psychotherapy
(671, 672) in minority groups, compared with Caucasians. If
treatment for depression is initiated, African Americans are
disproportionately more likely to receive pharmacotherapy (672), to drop out of treatment (673), and to develop
chronic symptoms (674) than are Caucasian patients.
These differences in mental health service use by minority
populations appear to have a number of potential causes.
Cultures and ethnicities may differ in the degree to which
psychiatric illness is stigmatized (675) and in the preferences of individuals for treatment (676–678). For example, studies have found that Hispanic individuals were
more likely to prefer counseling than whites, whereas African Americans varied across studies in their relative
preference for counseling rather than pharmacotherapy
(6, 679). Service use by minority populations is more affected by financial constraints (including those related to
insurance) and social barriers (e.g., stigma) than the use of
comparable services by Caucasians (664, 680, 681). In addition, pharmacological factors may play a role in patient
preferences and adherence, as ethnic groups may differ in
their relative rates of metabolism (682–684) and side effects and response to antidepressant medications (685–
688).
4. Older age
The combined prevalence of major depression, dysthymic
disorder, and “minor” depression in individuals over age
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
60 years has been reported to be as high as 25%, and major depressive disorder has been reported to be present in
14%–42% of nursing home residents (689). Elderly patients typically display more vegetative signs and cognitive disturbance but report less subjective dysphoria than
younger patients. Major depressive disorder may consequently be misattributed to physical illness, dementia, or
the aging process itself. For older adults with chronic
illness or physical disability, including those expected to
remain in a long-term care facility, depression may be erroneously regarded as expected or inevitable, and therefore
untreatable (690). As a result, it is common for major depressive disorder to be undiagnosed and untreated among
older adults.
As in all depressed individuals, a suicide risk assessment
is an essential element of the evaluation process in older
individuals. Although older adults constitute only 13% of
the U.S. population, they account for 19% of all suicides,
with elderly white men having the highest rates of completed suicides (691). This increase in suicide risk with aging in some demographic groups should be taken into
consideration when estimating suicide risk and developing a plan to reduce such risk.
Several general medical conditions common among
older adults are risk factors for depression. In addition,
the presence of depression often exacerbates the course of
the co-occurring medical condition and is a risk factor for
poor outcomes. For example, elderly patients who are depressed and recovering from hip fractures have poorer
functional outcomes from rehabilitative care and are less
likely to return to full ambulation, compared with older
adults with hip fractures who are not depressed (692–
694). There is also frequent co-occurrence of major depressive disorder and cardiovascular disease; 25% or more
of those with cardiovascular disease also have major depressive disorder, and co-occurring depression increases
the morbidity and mortality of cardiovascular illness
(695–697). The term vascular depression has been used to
describe depression occurring in late life in patients with
clinical evidence of cerebrovascular disease (698), although at this time it has not been established as a unique
subtype of depression. In addition, major depressive disorder is a complication of cerebral infarction (see Section
III.C.3). There is also a high prevalence of major depressive disorder among patients with dementia, and mood
symptoms may precede cognitive symptoms and diagnosis of dementia (see Section III.A.3.C).
Just as patients with medical conditions should be
screened for depression, patients exhibiting symptoms of
depression should be thoroughly evaluated for the presence of co-occurring medical conditions, as major depressive disorder and general medical illnesses frequently
67
coexist, especially in elderly patients (696, 699). This evaluation should include a systematic review of the patient’s
medications. Some medications have been reported to induce depressive symptoms (e.g., beta-blockers), although
they may simply be producing lethargy and fatigue that
mimic depression (700, 701). Consequently, the psychiatrist must carefully assess whether a given medication is
contributing to depressive symptoms before prematurely
altering what may be a valuable treatment. Patients undergoing their first major depressive episode in old age
should be assessed for an undiagnosed neurological or
other general medical disorder that may be responsible
for the depressive symptoms. Similarly, frequently cooccurring symptoms of major depressive disorder, such as
lassitude or pain, may mimic symptoms of a general medical condition. Pain in older adults, especially from orthopedic sources, may contribute significantly to the presence
of depression in this population (702).
Once the patient has been thoroughly assessed, the
treatment considerations for depressed geriatric patients
are essentially the same as for younger patients. A metaanalysis has shown that SSRIs; TCAs; and cognitivebehavioral, behavioral, and psychodynamic therapies are
all superior to placebo in the acute treatment for depression in subjects older than age 55 years (703–708). In addition, treatments for depression have been shown to be
effective in nursing home populations (709, 710), as well
as in inpatient and traditional outpatient settings of care.
However, compared with younger individuals, older patients may be more likely to experience relapses and less
likely to achieve a full response to treatment with antidepressant medications (711–714). In contrast, ECT is not
only effective as a treatment for depression among older
individuals, but those over age 65 years actually have better response rates than younger patients (715). Consideration should also be given to combined treatment with
pharmacotherapy and psychotherapy, as evidence for the
efficacy of stand-alone psychotherapy, such as CBT, is
weak (716). Although the role of stimulants for antidepressant monotherapy is very limited, these compounds
have some role in apathetic major depressive disorder in
elderly patients with complicating general medical conditions. Late-life depression associated with vascular disease
has also been found to respond well to treatment with antidepressants (717) and, in one unreplicated study, to
TMS (718). Furthermore, in a recent randomized controlled trial, administering escitalopram prophylactically
to patients who had experienced a stroke resulted in
lower rates of depression at 12 months (334). Psychosocial factors are also frequent contributors to depression
among older adults and should be addressed as part of the
treatment plan (719, 720).
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68
There are several considerations in prescribing medications for elderly patients. As with any patient, the psychiatrist should attempt to use as few medications as possible,
and this is especially important given the complexity and
multiplicity of issues in elderly patients. It is often useful
to use medications that address several issues at once, such
as choosing mirtazapine for a depressed, elderly patient with
weight loss and insomnia. Elderly patients typically require
a lower oral dose than younger patients to yield a particular blood level, and they tolerate a given blood level less
well. Nevertheless, the blood levels at which antidepressant medications are maximally effective for elderly patients appear to be the same as those for younger patients
(721, 722). Dose regimens should be adjusted for agerelated metabolic changes, with close attention paid to
hepatic and renal metabolic function. For patients who
are receiving other medications, careful attention should
be paid to potential drug interactions (160, 161, 723–725)
(Tables 4 and 5).
Elderly patients are particularly prone to orthostatic
hypotension and cholinergic blockade; for this reason,
SSRIs, SNRIs, and other antidepressants should be considered over MAOIs or TCAs. Among the TCAs, desipramine and nortriptyline should be considered over
amitriptyline, imipramine, and doxepin, due to increasing sensitivity to side effects and toxicity with advancing
age. Treatment with SSRIs causes the syndrome of inappropriate antidiuretic hormone secretion (SIADH) at a
higher rate in elderly patients than in younger patients (726,
727). Patients taking SSRIs have a three times greater risk
of developing SIADH than patients taking other antidepressants, with the greatest risk among elderly patients
(728).
For maintenance treatment, one study has shown that
antidepressant medication (nortriptyline) and IPT are effective for elderly patients with recurrent major depressive disorder (315), yet a trend toward superior response
was observed for combined pharmacotherapy and IPT,
compared with pharmacotherapy alone. Another study
demonstrated that paroxetine (but not monthly psychotherapy) was effective as maintenance therapy for elderly
patients (729). For older patients with particularly severe or treatment-resistant depressive illness, addition of
maintenance ECT to nortriptyline appears to improve
treatment outcome (730). Among elderly patients who
have had prior depression, the risk of developing another
episode of major depressive disorder is substantially increased in those who develop or report sleep disturbance
(731). Sleep disturbances may function as independent
predictors of depression and are not simply prodromal depressive symptoms.
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A body of systematic evidence suggests a particular
value for various forms of collaborative or team-based
care for elderly patients. Such care combines, for example,
specialty mental health consultation/intervention with
primary care management or community-based outreach
and monitoring of care (732, 733). Older adults with depression can benefit from integration of mental health
services in the setting where they typically receive their
general medical care. It has been shown that support for
algorithm-driven depression care processes within the
primary care outpatient practice can lead to increased
treatment adherence and improved clinical outcomes, including a reduction in mortality (734).
5. Gender
As part of the diagnostic assessment of a woman with major depressive disorder, there should be a detailed inquiry
regarding reproductive life history and mood symptoms
associated with reproductive life events, such as menses,
use of oral contraceptive agents, peripartum, infertility,
menopause, and pregnancy loss due to abortions, miscarriages, and perinatal losses. Although associations between reproductive factors and major depressive disorder
are neither widespread nor consistent, some women may
be particularly vulnerable to fluctuations in gonadal hormone levels (735). The perimenopausal transition has
been identified as a high-risk period for new-onset major
depressive disorder, with high variability of sex hormones
as a risk factor (736, 737). Women in the perimenopausal
transition may benefit from the use of serotonergic antidepressants, for mood and also for somatic symptoms such
as hot flashes (738).
Since women are often caretakers in families, psychosocial stresses such as caring for an ill husband, child, or
parent must be carefully assessed. Treating depressed
mothers is associated with improved prognosis for their
children as well (739). Maternal remission from depression
was associated after 3 months with significantly decreased
diagnoses and symptoms in their children, compared with
children of mothers whose depression had not remitted.
Thus, treating depressed mothers may crucially benefit
both the patients and their children.
The patient’s gender also factors into other treatment
considerations for major depressive disorder. For example, the risks of certain adverse effects from treatments
may also differ by gender. When prescribing trazodone to
men, it is important to provide education about the risk of
priapism (174). Older men typically have prostatic hypertrophy, making them particularly sensitive to anticholinergic effects of some antidepressants on the bladder
outlet. While both men and women may experience de-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
creased libido or anorgasmia while taking SSRIs, men
may also experience ejaculatory dysfunction (740). Some
women who are taking birth control pills require higher
doses of TCA medications because of the induction of the
hepatic enzymes responsible for medication metabolism.
Similarly, medications that induce hepatic enzymes, such
as anticonvulsants used as adjunctive treatment, reduce
the effectiveness of contraceptives.
6. Pregnancy and postpartum
Major depressive disorder during pregnancy and postpartum presents unique treatment considerations. During
these periods, approximately 10% to 15% of perinatal
women will experience major depressive disorder, which
is at least as common as rates reported for women in nonreproductive states (741, 742). Evaluation and communication of risks and benefits of antidepressants during
pregnancy and breast-feeding is challenging and must include the risks of untreated maternal mood disorder, the
limited body of research that informs safety of antidepressants, and the general lack of prospective long-term data
following antidepressant exposure in utero and through
lactation.
Depression-focused psychotherapy or other nonmedication therapies may be considered first for some women,
and psychotherapy should be considered as part of the
treatment plan whenever possible. As childbearing is a life
stressor with psychosocial repercussions that may be amenable to psychotherapy, psychotherapy may serve to minimize medication exposure in some women. Although
there is little controlled research, psychotherapies appear
efficacious in antenatal and postpartum depression, with
IPT being the best studied (743, 744). Therefore, depression-focused psychotherapies such as IPT and CBT
should be considered in the treatment plan as a first-line
treatment or in combination with medication to minimize
medication exposure, especially if the individual has experienced a good response to a particular psychotherapy in
the past or strongly prefers to avoid medication.
a. Depression during pregnancy
Psychiatrists should be familiar with the management of
major depressive disorder in the context of pregnancy
(745). More than 80% of women in the United States will
have children (746), and about half of pregnancies are
unplanned (747). Therefore, pregnancies—including unplanned pregnancies—are likely to occur during the course
of treatment of major depressive disorder, as it is often a
chronic and/or recurrent condition that is a major cause
of disability during the reproductive years and disproportionately affects women, compared with men. In consid-
69
eration of the high prevalence of both unplanned pregnancy
and major depressive disorder in women, the risks and
benefits of antidepressants and untreated maternal depression during pregnancy should be discussed with all female patients who have reproductive potential. Whenever
possible, a pregnancy should be planned in consultation
with a treating psychiatrist, who may wish to consult with
a specialist in perinatal psychiatry. For women who are
pregnant or planning to become pregnant, decisions
about treatment for depression require weighing multiple
benefits and risks for the woman as well as for the fetus.
Making such decisions may require several discussions
and will generally involve discussions with the patient’s
partner as well as her obstetrician.
Antidepressant medications carry some reported risks
in pregnancy (see below), but so does untreated depression. Suicide risk, marital discord, the inability to engage
in appropriate obstetrical care, and difficulty caring for
other children must also be considered. There are also serious and well-characterized risks to the fetus of exposure
to maternal major depressive disorder, including the possibility of low birth weight secondary to poor maternal
weight gain (or frank weight loss) and increased risk of obstetrical complications such as premature delivery (748).
Antidepressant efficacy has not been determined for
pregnant women, and questions remain as to whether
medications have equivalent efficacy during pregnancy,
compared with the nonpregnant state. Some safety data
are available, but the findings often conflict, making data
interpretation challenging and difficult to apply to the
care of individual patients. Nevertheless, antidepressant
medication should be considered and discussed as an option with pregnant women who have moderate to severe
major depressive disorder.
For women who are in remission from major depressive disorder and receiving maintenance medication
and/or for women deemed to be at high risk for a recurrence if the medication is discontinued, the risks of treatment with medications must also be weighed against the
risks of alternative treatment options and untreated depression. Relapse rates for women with a history of major
depressive disorder are high during pregnancy, especially
if antidepressants are discontinued (749).
1. Risks of antidepressants during pregnancy
The impact of the duration and timing of antidepressant
exposure during pregnancy requires further study. Wisner
et al. (750) reviewed the risks associated with the use of
antidepressants during pregnancy, and a growing body of
complicated literature has followed. Overall, risk of teratogenicity with antidepressants following first trimester
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70
exposure appears to be low, although some rare birth defects have been observed to occur at higher rates with use
of specific SSRIs (751, 752). First-trimester paroxetine
exposure has been associated with cardiac malformations,
a finding that resulted in changes in FDA labeling for paroxetine from C to D (753); labeling changes have been
made to all SSRI antidepressants with regard to this possibility when used during pregnancy. There have been
conflicting results regarding whether first-trimester paroxetine exposure and cardiac teratogenicity are associated
(754, 755). For fluoxetine, one study (756) found a higher
incidence of three or more minor physical anomalies in
infants exposed to fluoxetine than in a control group, and
fetuses exposed to fluoxetine after 25 weeks’ gestation had
lower birth weights, which were associated with lower
maternal weight gain. Although one case-control study
reported a potential association between late antenatal
SSRI use and the rare but serious condition of persistent
pulmonary hypertension in the newborn (PPHN) (757),
two subsequent retrospective chart review studies showed
no such association (758, 759). An additional case-control
study (760) showed a marginally significant increase in the
relative risk of PPHN with SSRI use, but the estimated
rate of PPHN occurrence was 1.5 per 1,000 births, which
is less than the rate of 2.7 per 1,000 births reported by others (758) in non-SSRI exposed infants. Therefore, while
many physicians are concerned about the reported association between SSRIs and PPHN, the preponderance of
evidence from published studies on this topic does not
support an association. Use of SSRIs may also be associated with prematurity (761, 762), although untreated depression and stress during pregnancy may also contribute
to the risk of prematurity (748, 763). Some naturalistic
studies and health care utilization studies suggest that
antidepressants are associated with shorter length of gestation (761, 762), but there have been no randomized studies of the treatment of antenatal major depressive disorder
that would adequately control for untreated maternal depression, antidepressant use, and confounding variables
related to treatment selection. With late pregnancy antidepressant use, some but not all studies show a risk of
medical complications such as prematurity and a transient
neonatal withdrawal/adaptation syndrome (761, 764). The
syndrome in the neonate appears to be associated with antidepressant use in the third trimester, has been reported
in babies exposed in utero to TCAs and SSRIs, and includes transient symptoms such as jitteriness, tremor, difficulty with feedings, and other symptoms (764). Several
studies, involving relatively small samples, have examined
effects of antidepressant exposure during pregnancy on
subsequent childhood behavior and development and
found minimal (765) or no (766–768) effects on language,
APA PRACTICE GUIDELINES
cognition, or motor or behavioral development independent of maternal depressed mood during pregnancy and
the child’s early life (766, 767).
2. Implementation of pharmacotherapy
during pregnancy
No controlled trials inform the use of antidepressants
during pregnancy. Dose requirements may change during
pregnancy because of changes in volume of distribution,
hepatic metabolism, protein binding, and gastrointestinal
absorption. Pharmacokinetic changes in late pregnancy
may result in lower blood levels, with clinical implications, although more study is needed to develop monitoring and dosing guidelines. The limited data in this area
demonstrate that pregnant women metabolize TCAs and
SSRIs more rapidly in late pregnancy (769–774).
A number of factors influence antidepressant choice
during pregnancy. If a woman has had a history of a good
response to or is already taking a particular antidepressant, it is logical to consider that antidepressant among
first-line treatments in an effort to minimize the number
of different medication exposures. Using a single agent is
also preferable to using several medications concomitantly. Because paroxetine use is classified as having a higher
level of risk than other SSRIs, it should not be considered
a first-line treatment when selecting a new antidepressant
for a pregnant patient. Fluoxetine has the longest half-life
and is more likely to be demonstrated at high levels in
newborns after in utero exposure. Sertraline has been
demonstrated to have lower cord blood levels than other
SSRIs, although the clinical significance of this is unknown (775). Although there are few data for bupropion
and safety in pregnancy, its benefits for smoking cessation
may make it especially useful in women who have major
depressive disorder and who smoke cigarettes, as tobacco
is a known teratogen. Given these data, it is recommended
that consideration be given to using an antidepressant
with some available safety information that has been
studied in pregnant women. For women who discontinue
medication during pregnancy and are deemed at risk for
postpartum depression, medication can be restarted following delivery.
Electroconvulsive therapy is also recommended as a
treatment option for major depressive disorder during
pregnancy (239). The current literature supports the
safety for mother and fetus, as well as the efficacy of ECT
during pregnancy (239). The psychiatrist should consider
ECT for pregnant patients with moderate to severe depression who are unresponsive to or unsuitable for pharmacotherapy, for pregnant patients with major depressive
disorder with psychotic features, and for pregnant patients electing to use this modality as a matter of prefer-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
ence after having weighed the relative risks and benefits of
ECT and other treatment options. For details on the use
of ECT during pregnancy, refer to The Practice of Electroconvulsive Therapy: Recommendations for Treatment, Training, and Privileging (A Task Force Report of the American
Psychiatric Association) (239).
b. Postpartum depression
Major depressive disorder with postpartum onset is defined in DSM-IV-TR as a major depressive episode with
onset within 4 weeks of delivery. However, the occurrence
and course of major depressive disorder in childbearing
women is heterogeneous, and definitions of postpartum
depression may evolve with continued research (16, 776).
In major depressive disorder with postpartum onset, anxiety symptoms are more prevalent than in major depressive disorder occurring at other times (777). It is not
uncommon for women with postpartum depression to
experience obsessions and/or compulsions, and obsessions may often involve thoughts of harming the baby,
which must be differentiated from postpartum psychosis.
Psychiatrists should provide psychoeducation about major depressive disorder to pregnant and postpartum
women and their families to improve the detection of major depressive disorder during pregnancy and the postpartum period.
Several other psychiatric conditions may follow childbirth (778). The transient 7- to 10-day depressive condition referred to as “postpartum blues” is by definition too
mild to meet the criteria for major depressive disorder and
does not require medication. In addition to providing reassurance, psychiatrists should encourage mothers who
experience postpartum blues to increase psychosocial support and obtain help with the care of the infant. Puerperal
psychosis is a more severe disorder complicating one to
two of 1,000 births. Although postpartum psychosis is
rare, women with this disorder may have homicidal impulses toward the newborn; for this reason, careful assessment of homicidal as well as suicidal ideation, intention,
and plans is important. Postpartum psychosis must always
be treated as a psychiatric emergency, with hospitalization
considered for the safety of the mother and baby (779).
Many patients who have had episodes of this type ultimately prove to have bipolar disorder (780).
The woman’s parenting skills for both the newborn
baby and any other children in her care must be carefully
assessed. Untreated maternal major depressive disorder,
and specifically postpartum depression, have negative
consequences for children, with adverse effects on attachment and child development (781, 782). Major depressive
disorder can seriously interfere with the new mother’s abil-
71
ity to provide physically and emotionally appropriate care
for her baby and other children. The psychiatrist should
work with the patient to develop a plan to manage this effect, such as enlisting family members to assist with child
care.
Antidepressants are often prescribed for postpartum depression, according to the same principles delineated for
other types of major depressive disorder, despite a limited
number of controlled studies. Two placebo-controlled trials of SSRIs (fluoxetine and paroxetine) have been published for the treatment of postpartum depression, with
fluoxetine appearing more efficacious than placebo and
paroxetine being comparable to placebo on primary outcome measures of depressive symptoms (783, 784). Wisner
et al. (785) did not find a difference in response and remission rates in a randomized controlled trial of sertraline versus nortriptyline for postpartum major depressive disorder.
Open studies of other antidepressants in postpartum
women suggest efficacy, although some studies included
only a small number of participants (786). Paroxetine alone
and paroxetine plus CBT both produced a significant change
from baseline in one study, but there was no placebo-only
group for comparison (787).
Patients and clinicians are often concerned about the
risks of possible exposure to antidepressants during
breast-feeding. These risks, however, must be weighed
against the well-known, and at times profound, risks to
the woman and her children of untreated postpartum
depression. Mothers should be counseled regarding the
relative risks and benefits when making these treatment
decisions. Antidepressant medications are considered
compatible with breast-feeding, but long-term data are
not available regarding risks and benefits. Although there
have been some suspected case reports of adverse effects
in breast-feeding infants exposed to maternal antidepressants, most studies show low levels of exposure via breast
milk, with the exception of fluoxetine, which appears to
have a dose-related risk for detectable levels in infant sera
(788, 789). At this time, there are no studies which have
determined a “safe” amount and duration of antidepressant exposure in the fetus and newborn. However, exposure to antidepressants via breast milk is considered
substantially lower than in-utero exposure. Women who
elect to breast-feed while taking antidepressants should be
supported in doing so, given the widely known health
benefits (e.g., immune system effects) to infants who are
breast-fed. Similarly, women who elect to bottle-feed
should also be supported in this decision. Some women
will not accept treatment with antidepressant medication
while they are breast-feeding. Depression-focused psychotherapy can be recommended instead.
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72
7. Family history
Major depressive disorder is one and one-half to three
times as common among those with a first-degree biological relative affected with the disorder as in the general
population. In addition, the rates of depression, anxiety,
and other disorders are increased more than two- to sixfold in the offspring of depressed parents. A family history
of depression is associated with an earlier age at onset of
depression (790), and children of depressed parents are
more likely to have depression with a chronic and recurrent course (791). Furthermore, a family history of recurrent major depressive disorder increases the chances that
the patient’s own illness will be recurrent and that the patient will not fully recover between episodes (792). A family history of bipolar I disorder, bipolar II disorder, or
acute psychosis probably increases the chances that the
patient’s own major depressive disorder is a manifestation
of bipolar rather than unipolar depression, and that antidepressant medication therapy may incite a switch to
mania (793). Patients with such a family history should be
questioned particularly closely regarding a prior history
of mania or hypomania and should be carefully observed
for signs of a switch to mania during treatment with antidepressant medication.
There are no real predictors of response to individual
antidepressants, yet in the absence of other information
clinicians sometimes rely on family history of therapeutic
benefit to select a specific medication for a family member. Although it does not have specific support in the literature, this practice appears reasonable.
C. TREATMENT IMPLICATIONS OF COOCCURRING GENERAL MEDICAL CONDITIONS
In patients with co-occurring medical conditions, there is
a higher prevalence of major depressive disorder than in
the general population. Furthermore, co-occurring medical conditions in patients with major depressive disorder
are associated with poorer outcome (794, 795). A number
of medical conditions are known to cause mood symptoms, such as stroke, hypothyroidism, carcinoma of the
pancreas, and many others. Apart from directly causing
depressive symptoms, debilitating, painful, and chronic
medical conditions often constitute an ongoing stressor
that predisposes patients to depressive episodes. Nevertheless, a depressive episode, in any context, is never a
“normal” response to illness and consequently warrants
treatment.
In addition to the increased risk of major depressive
disorder with general medical conditions, depressive episodes increase the risk of certain general medical conditions,
APA PRACTICE GUIDELINES
such as heart disease. (796). Due to the interrelationship
between depression and medical illness, it is very important to recognize and treat depressive symptoms in medically ill patients, and vice versa. The psychiatrist should
also attend to the potential for interactions between antidepressants and the co-occurring medical conditions as
well as any nonpsychiatric medications that the patient
may be taking.
1. Hypertension
The presence of treated or untreated hypertension may influence the choice of an antidepressant, as a few antidepressant medications have been associated with increases in
blood pressure. With SNRIs such as venlafaxine and duloxetine, dose-dependent elevations in blood pressure are
usually mild, although more severe hypertension has also
been observed (166, 797). However, another study found
no increase in hypertension with duloxetine dosed up to
80 mg/day (798). Hypertension induced by SNRIs may respond to a decrease in the medication dose, or an alternative
antidepressant medication may be considered. Alternatively, for a patient with well-controlled depressive symptoms, it may be preferable to add an antihypertensive agent
rather than risk a depressive relapse or recurrence with
medication tapering.
Antihypertensive agents and antidepressant medications may interact to either intensify or counteract the effect of the antihypertensive therapy (799). The action of
antihypertensive agents that block alpha receptors (e.g.,
prazosin) may be intensified by antidepressant medications that block these same receptors, notably the TCAs
and trazodone. Tricyclic antidepressants may antagonize
the therapeutic actions of guanethidine, clonidine, or alpha-methyldopa. Concomitant antihypertensive treatment, especially with diuretics, increases the likelihood
that TCAs, trazodone, or MAOIs will induce symptomatic
orthostatic hypotension.
Side effects of antihypertensive agents, such as fatigue
or sexual dysfunction, may also confound the evaluation
and interpretation of depressive symptoms. It has also
been thought that beta-blockers, especially propranolol,
may account for depressive symptoms in some patients,
but this association has been questioned (700, 701).
2. Cardiac disease
Depression increases the risk of cardiovascular disease
(800). In addition, patients who are depressed following a
myocardial infarction have an increased rate of mortality,
compared with patients without depression (801–803).
Following an acute myocardial infarction, the decreased
survival rates of depressed patients may in part be due to
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
lower heart rate variability in these patients, compared
with nondepressed patients (804). Particularly in patients
with a history of major depressive disorder (805), there is
evidence that the depressive symptoms associated with
cardiac illness respond to antidepressants (717, 806, 807).
However, studies in which the attempt has been made to
influence cardiac-related mortality through treatment of
depression have shown mixed results (808–811).
A depressed patient with a history of a cardiac problem
should be monitored for the emergence of cardiac symptoms, ECG changes, persistent tachycardia, or orthostatic
blood pressure decrements. Consultation with the patient’s cardiologist before and during antidepressant medication treatment may be advisable, especially for patients
who have recently had a myocardial infarction. Increases
in heart rate and blood pressure may be associated with
the use of agents with noradrenergic properties such as
SNRIs and stimulants; thus, changes in heart rate and blood
pressure should be assessed after treatment with these
agents is instituted in patients with coronary artery disease, hypertension, or congestive heart failure. Although
TCAs have been used effectively to treat major depressive
disorder in patients with some forms of ischemic heart
disease (812), psychiatrists should take particular care in
using TCAs for patients with a history of ventricular arrhythmia, subclinical sinus node dysfunction, conduction
defects (including asymptomatic conduction defects), prolonged QT intervals, or a recent history of myocardial infarction (184, 185, 813–818). Selective serotonin reuptake
inhibitors, SNRIs, and bupropion appear to be safer for
patients with preexisting cardiac disease; several SSRIs
have been used safely in patients with cardiac disease in
large clinical trials (807, 809, 810, 819). Electroconvulsive
therapy can also be used safely in individuals with cardiac
disease or arrhythmias, although specialist consultation
and modifications in ECT technique or anesthesia may be
indicated (239, 245, 820–822). Monamine oxidase inhibitors do not adversely affect cardiac conduction, rhythm,
or contraction but may induce orthostatic hypotension
and have risks relating to drug-food and drug-drug interactions.
3. Stroke
Depression is observed in approximately one-third to
one-half of individuals in the weeks to months following a
stroke, with a substantial proportion developing major
depressive disorder (334, 823, 824). Although conclusions
of meta-analyses are mixed (825, 826), some research
suggests that antidepressant treatment immediately following a stroke may reduce rates of depression (334) and
possibly mortality (827). Among psychotherapeutic ap-
73
proaches to preventing depression after stroke, problemsolving therapy has been best studied, but findings are inconsistent (334, 825).
When depression develops after a stroke, it has detrimental effects on quality of life (823). In addition, the
presence of depression 1 month following a stroke has
been associated with an increase in subsequent mortality
(828). Use of screening tools such as the PHQ-9 may help
to identify depressive episodes after stroke (829), and care
management may improve outcomes once poststroke depression is recognized (830). Psychotherapies have not
been well studied as treatments for poststroke depression;
however, a meta-analysis of randomized trials that have
been conducted did not show efficacy (825). Findings on
the therapeutic effects of antidepressants in post-stroke
depression have been mixed, perhaps due to the substantial heterogeneity of study populations and designs (831,
832). Although a meta-analysis did not show any difference in the rate of depressive remission with antidepressant treatments compared with placebo (832), patients
receiving an antidepressant did show more improvement
in depressive symptoms (831, 832) and a greater proportion were classified as treatment responders (831). Individual randomized controlled trials have shown therapeutic
benefits for several SSRIs, including fluoxetine, sertraline,
and citalopram (833–836), and for the TCA nortriptyline
(837, 838); however, not all studies have shown benefit for
some of these agents (837, 839–841). Nevertheless, for individuals with poststroke depressive symptoms, a trial of
antidepressant therapy may be considered, with SSRIs
being better tolerated and having fewer contraindications
in this older and more medically ill population (842, 843).
However, in individuals who are receiving concomitant
treatment with anticoagulant (e.g., warfarin) or antiplatelet
(e.g., dipyridamole, clopidogrel, aspirin) medications, it is
important to consider the potential for an increased bleeding risk due to drug-drug interactions with antidepressants (844, 845).
4. Parkinson’s disease
Major depressive disorder occurs to some degree in 40%–
50% of patients with Parkinson’s disease. Patients with
Parkinson’s disease experience alterations of serotonergic
and noradrenergic systems that may induce depression.
There is no evidence favoring any particular antidepressant medication from the standpoint of therapeutic efficacy and safety for patients with Parkinson’s disease
complicated by major depressive disorder (846). A metaanalysis of placebo-controlled studies identified a clear
benefit for both active treatment and placebo, but it did
not find differences between them (847). Although SSRIs
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74
can be used, there is some risk of worsening of Parkinson’s
disease symptoms (increases in “off” time and exacerbation of tremor) with agents that are primarily serotonergic
(848). Bupropion, in contrast, exerts a beneficial effect on
the symptoms of Parkinson’s disease in some patients but
may also induce psychotic symptoms, perhaps because of
its agonistic action in the dopaminergic system (849).
Noradrenergic agents and SNRIs may also be preferable
to SSRIs. Nonselective MAOIs (e.g., tranylcypromine,
phenelzine, isocarboxazid) may adversely interact with Ldopa products (850). Selegiline, also known as L-deprenyl, is a selective type B MAOI recommended in the treatment of Parkinson’s disease. Selegiline loses its specificity
for MAO B in doses greater than 10 mg/day. As a result, it
may induce serotonin syndrome when given in higher
doses in conjunction with serotonin-enhancing antidepressant medications. The theoretical benefits of the antimuscarinic effects of some of the tricyclic agents in the
treatment of patients with major depressive disorder with
Parkinson’s disease are offset by the memory impairment
that may result. Amoxapine, an antidepressant medication
with dopamine-receptor-blocking properties, should be
avoided for patients who have Parkinson’s disease. Lithium may, in some instances, induce or exacerbate parkinsonian symptoms. Electroconvulsive therapy exerts a
transient beneficial effect on the symptoms of idiopathic
Parkinson’s disease in many patients (851, 852); however,
it might occasionally worsen L-dopa-induced dyskinesias
and induce a transient interictal delirium (853), which necessitates reductions in doses of dopamine agonist medications (239).
5. Epilepsy
The prevalence of depression in individuals with epilepsy
appears to be increased in secondary and tertiary care center samples, although in population-based studies this increase is not well established (854). On the other hand,
major depressive disorder significantly increases the risk
of unprovoked seizures even after the adjustment of age,
sex, length of medical follow-up, and medical therapies
for depression (855). In addition, some antidepressant
drugs, such as TCAs and bupropion, lower the seizure
threshold and have a dose-dependent epileptogenic potential. This seizure risk is intermediate for immediaterelease formulations of bupropion, maprotiline, and
TCAs (in particular, clomipramine) and low for sustainedrelease formulations of bupropion (17, 197, 856).
Major depressive disorder in patients with seizure disorders can usually be safely and effectively managed according to the same principles outlined for patients
without seizures. In particular, SSRIs and SNRIs are not
APA PRACTICE GUIDELINES
likely to increase the risk of developing seizures (856–
858). However, blood levels of TCAs may be increased by
several antiepileptic drugs, increasing the side-effect burden of the anticholinergic and other side effects of tricyclics (859).
Some anticonvulsants appear useful for treatment and
prophylaxis of mood disorders (e.g., carbamazepine, valproate, lamotrigine). Thus, in patients with depression and
epilepsy, consideration can be given to concomitant prescription of an anticonvulsant (or elevating the dose of an
existing anticonvulsant). Nevertheless, anticonvulsant compounds may also have a negative effect on mood for some
patients (859). For example, barbiturates and possibly vigabatrin have been associated with an increased risk for
depression (860). In addition, a recent FDA statement noted
that increased rates of depression and suicide risk may be
associated with anticonvulsants (861).
6. Obesity
Many individuals with major depressive disorder will be
overweight or obese, given the high prevalence of excess
weight in the general population (862). In addition, rates
of depression may be increased in obese individuals, particularly among women and in those with a body mass index (BMI) greater than 40 (863). Individuals with obesity
resulting from binge eating disorder also have higher rates
of depression (170). In the subgroup of patients with atypical depression, increased eating and weight gain are
symptomatic of the depressive disorder (864). For other
patients, the lack of motivation and energy that occur with
depression can make it difficult to maintain an exercise
regimen or nutritional dietary habits. In addition, treatment with many antidepressant medications appears to
lead to weight gain (865) and also makes it more difficult
to lose weight in a structured weight management program
(866).
In treating individuals with major depressive disorder
who are overweight or obese, the effects of treatment on
weight should be considered in selecting a therapeutic approach. If pharmacotherapy is used, the selection of an antidepressant medication should include consideration of
its relative tendency to contribute to weight gain, which
is generally greatest with mirtazapine, TCAs (tertiary
TCAs more so than secondary TCAs), and MAOIs and
less prominent with SSRIs and SNRIs (865). Bupropion is
generally weight neutral and has been associated with
modest weight reduction when used to treat major depressive disorder in obese adults (867, 868). Longitudinal
monitoring of weight, either by direct measurement or
patient report, can permit monitoring of BMI, as well as
early intervention if weight gain becomes a problem with
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
antidepressant treatment. Patients’ concerns about weight
gain may also contribute to poor adherence, and monitoring of weight can facilitate such discussions. The impact
of weight on medication dosing should also be considered. In one study, greater relative body weight was associated with a lesser likelihood of response to a fixed dose
trial of an antidepressant (869), perhaps suggesting a need
for increases in medication dose with increasing body
weight.
Psychotherapeutic approaches to treatment avoid the
potential for medication-induced weight gain and may
also have modest benefits in weight management. Cognitive-behavioral therapy has shown efficacy in the treatment of binge eating disorder (170, 870) and could
potentially be used in addressing obesity (871) and medication-induced weight gain (872).
The increasing use of surgical treatments for obesity
also has implications for the treatment of patients with
major depressive disorder. Depression is common among
bariatric surgical candidates and, in and of itself, is not a
contraindication for surgery (873–877). Long-term follow-up studies show improvements in co-occurring general medical conditions (878), as well as decreases in
depressive symptoms and improved quality of life with
weight loss (879–881). However, weight loss after surgery
may be less pronounced in individuals with a lifetime diagnosis of major depressive disorder (882) or in those with
severe psychiatric illness that has required hospitalization
(883). Close follow up is important following bariatric
surgery in order to assess for changes in psychiatric symptoms, assist patients in the psychological and psychosocial
adaptation to weight loss, and adjust medication regimens. Particularly following jejunoileal bypass or biliopancreatic diversion, but also following gastric bypass
procedures, altered dissolution (884) and absorption of
medication may require adjusting the dose of medication
or changing from a slow-release to an immediate-release
formulation (875).
75
significant dosing adjustments, it is useful to collaborate
with the patient’s primary care physician in monitoring
diabetic control because fluctuations in fasting blood glucose may occur. Some evidence suggests that use of TCAs
may be associated with worsened glycemic control, and
other antidepressants (such as SSRIs) may be preferable to
TCAs for patients with diabetes (896, 897).
8. Sleep apnea
The possible contribution of obstructive sleep apnea (OSA)
to depressive symptoms is an important consideration, particularly in patients who are obese, report excessive daytime
sleepiness, or have treatment-resistant depressive symptoms. Symptoms such as fatigue and poor sleep quality can
occur in sleep apnea as well as in major depressive disorder,
requiring a careful assessment to distinguish whether either
or both disorders are present. Underrecognition of OSA is
common, and rates of OSA appear to be increasing with the
increasing prevalence of obesity (898). Although the prototypical sleep apnea patient is likely to be obese with a history of snoring, sleep apnea may still be present even in the
absence of these findings (899). Individuals with OSA or
excessive daytime sleepiness appear to have greater rates of
depression than comparison groups (900–902), although the
rates of depressive symptoms and major depressive disorder diagnosis fluctuate across studies (903). In addition, epidemiological findings suggest an increasing likelihood of
depression with increasing sleep-related breathing disorder
severity (904). With initiation of continuous positive airway
pressure treatment, improvement in OSA symptoms has
been associated with decreased depressive symptoms (905,
906), in addition to reductions in OSA-associated health
risks (898). Consequently, recognition and treatment of
OSA is important among individuals with major depressive
disorder. Identification of OSA is also important to treatment planning, as use of sedating medications can exacerbate OSA and worsen daytime sleepiness, with associated
complications (907).
7. Diabetes
9. Human immunodeficiency virus and hepatitis C infections
Diabetes mellitus is common in the general population,
particularly in overweight or obese individuals (885).
However, it is not clear whether an association exists between diabetes and major depressive disorder, as metaanalyses and epidemiologic studies yield mixed results
(886–888). Some patients may have reduced adherence to
diet and medications when depressed (889), but there are
inconsistent findings on whether successful treatment of
depression (with medication, psychotherapy, and/or collaborative care) improves glycemic control (889–896). However, when initiating antidepressant therapy or making
According to the Centers for Disease Control and Prevention, more than one million individuals in the United
States were living with HIV infection by the end of 2003
(908), with increased rates among individuals with psychiatric disorders, including substance use disorders (909).
Estimates suggest that at least one-fifth of infected individuals have unrecognized infection (910), necessitating
increased efforts to identify HIV infection (911), given
the availability of effective treatment (912). Consequently,
clinicians treating patients with major depressive disorder
should consider screening for HIV.
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Rates of major depressive disorder are increased among
individuals with HIV infection, compared with HIV-negative individuals (913). When treating major depressive disorder in patients who also have HIV, antidepressant
medications can be used safely and effectively (914, 915),
although high placebo response rates and high study attrition rates have sometimes confounded interpretation of research findings (916, 917). When antidepressants are used,
SSRIs are better tolerated than TCAs (918, 919). In individuals who are receiving treatment with antiretroviral
agents, it is important to check for potential drug-drug interactions when choosing a medication regimen (920). Significant interactions can also occur if St. John’s wort is taken
by patients receiving antiretroviral medications. Although
few studies have been conducted in patients who meet diagnostic criteria for major depressive disorder, individual
and group psychotherapies using interpersonal, cognitivebehavioral, and psychoeducational approaches have also
been associated with reductions in depressive symptoms
among patients with HIV infection (316, 921–926).
Persons with mental illness also have elevated rates of
infection with hepatitis C (927), and infection with hepatitis C is commonly present in individuals with HIV infection (928). Among individuals with hepatitis C, depressive
symptoms are common, and many patients fully meet the
criteria for major depressive disorder (929). Treatment of
hepatitis C with interferon appears to be associated with a
further increase in the risk for depression, although findings vary depending upon the study population, concomitant medications (e.g., ribavirin), and the type of interferon
used for therapy (930, 931). The increase in depressive
symptoms with interferon treatment may also be more
prominent in patients with greater levels of pretreatment
depression (932). This suggests a need for careful monitoring if patients with current major depressive disorder are
administered interferon, particularly since many patients
treated with interferon have unrecognized or insufficiently
treated depression (933). Studies in which antidepressant
medications were administered concomitantly with interferon have shown inconsistent prophylactic effects (934,
935). However, antidepressant therapy does seem to be effective when used to treat depression that develops in the
course of interferon therapy for hepatitis C infection (936,
937). Consequently, major depressive disorder should not
be viewed as a contraindication to the treatment of hepatitis
C infection, particularly given the severe long-term hepatic
complications associated with chronic infection (938).
10. Pain syndromes
Pain syndromes and major depressive disorder frequently
co-occur. Although the reported prevalence of pain
among depressed patients varies with cultural differences
APA PRACTICE GUIDELINES
and study design, one-half to two-thirds of depressed individuals will typically note some type of pain (702, 939–
941). Conversely, in primary care settings, individuals
with pain symptoms are about twice as likely to be depressed as those without pain, and the rates of depression
are further increased if pain is chronic or involves multiple
types of pain (940, 942). It is important to note that individuals with co-occurring pain and depression tend to
have worse treatment outcomes and poorer overall functioning than those with either condition alone (940, 942–
944). Consequently, every patient with depression should
be assessed for the presence, nature, location, and severity
of pain complaints.
Overall, antidepressant treatment has been associated
with reductions in pain symptoms among individuals with
psychogenic or somatoform pain disorders (945). However, among trials of second-generation antidepressants in
individuals with co-occurring pain and depression, duloxetine, venlafaxine, and paroxetine seem to be of comparable but relatively minor benefit (939, 946, 947).
Neuropathic pain is commonly associated with diabetic
peripheral neuropathy but may also have other etiologies
such as postherpetic neuralgia. For neuropathic pain in
general, evidence-based guidelines recommend the use of
TCAs or SNRIs (948, 949). Of the antidepressant medications, TCAs have been found to be most effective in decreasing pain associated with both postherpetic neuralgia
(950, 951) and diabetic neuropathy (949, 952) but have no
apparent effect on HIV-associated neuropathic pain (949).
Given the greater tolerability of SNRI antidepressants,
these agents may sometimes be chosen before a TCA for a
patient with co-occurring depression and neuropathic pain.
In addition, if a TCA is used, therapeutic drug monitoring
may be helpful, given the wide variability of TCA blood
levels across individuals (953).
Similar effects have been found for the use of antidepressants to prevent migraine and tension-type headaches.
In patients with and without co-occurring depression,
TCAs show greater efficacy than SSRIs (954, 955), but
SNRIs also have some evidence for efficacy (956, 957). In
individuals with tension-type headaches, addition of stress
management therapy may augment the effects of TCA
treatment (958).
Antidepressant treatment is also recommended for individuals with fibromyalgia, as it is associated with reductions in pain and often leads to improvements in function,
with the best evidence available for amitriptyline (959).
Beneficial effects are observed in those with or without
co-occurring major depressive disorder (960–962). Although evidence from controlled trials is more limited for
nonpharmacological approaches than for antidepressant
treatment, education, exercise, and CBT are generally rec-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
ommended for the treatment of fibromyalgia in combination with antidepressant medication (963, 964).
In the context of rheumatoid arthritis, antidepressant
medications also appear to be effective in reducing pain as
well as treating depressive symptoms (965–967). Evidence
for psychosocial treatment is less consistent, with mindfulness meditation and emotion regulation therapy being
associated with reduced pain and enhanced coping in individuals with rheumatoid arthritis and depression (968),
but CBT having mixed results (966, 968). In individuals
with co-occurring depression and osteoarthritis, collaborative depression care has been associated with reduced
pain severity, improved function, and enhanced quality of
life in those with low pain scores at baseline but had no effect when compared with usual treatment in those with
severe arthritis pain (969, 970).
For individuals with chronic low back pain, there are
conflicting opinions about the utility of antidepressant
medications in reducing pain or improving function, even
in the presence of co-occurring depression (971, 972).
Nevertheless, antidepressant medications may still be indicated to treat depression on the basis of individual circumstances.
Since depressed patients with concurrent pain are often treated by primary care physicians and other medical
specialists with a variety of potent analgesic medications,
including narcotics, psychiatrists treating such patients
are advised to be in contact with these other physicians
initially and on a regular ongoing basis as indicated. The
purposes of such contacts are to review the entire treatment plan, to assure that all prescribing physicians are
aware of the full extent of pharmacological interventions,
to coordinate specific prescribing areas and responsibili-
77
ties so that patients do not receive prescriptions for the
same medications or have their doses for given medications adjusted by several different prescribing clinicians,
and to set up a mechanism and plan whereby all prescribing clinicians consistently keep one another informed
about changes in their treatment plans and prescriptions.
11. Obstructive uropathy
Enlarged prostate size and other causes of bladder outlet
obstruction are relative contraindications to the use of antidepressant medication compounds with antimuscarinic
effects. For this reason, tertiary amine TCAs are best
avoided in these patients. Benzodiazepines, trazodone,
and MAOIs may also retard bladder emptying. The antidepressant medications with the least propensity to do
this are SSRIs, SNRIs, and bupropion. If a TCA is chosen,
the secondary amine desipramine is the least likely to
cause urinary hesitancy or retention.
12. Glaucoma
Medications with anticholinergic potency may precipitate
acute narrow-angle glaucoma in susceptible individuals
(i.e., those with shallow anterior chambers) (973). Patients
with glaucoma receiving local miotic therapy may be
treated with antidepressant medications, including those
possessing anticholinergic properties, provided that their
intraocular pressure is monitored during antidepressant
medication treatment. Prescription of agents lacking
anticholinergic activity avoids this risk. Other agents
sometimes used in psychiatry, e.g., topiramate and related
sulfa-based medications, may cause acute angle closure
glaucoma by ciliary body edema, a different mechanism
(974).
Part B
BACKGROUND INFORMATION AND REVIEW
OF AVAILABLE EVIDENCE
IV.
DISEASE DEFINITION, EPIDEMIOLOGY, NATURAL HISTORY,
AND COURSE
A. DISEASE DEFINITION
The DSM-IV-TR criteria for major depressive episode and
major depressive disorder are listed in Table 11. The cardi-
nal feature of a major depressive episode is either a depressed mood or loss of interest or pleasure in usual activities that persists over a period of at least 2 weeks and is
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78
accompanied by a constellation of depressive symptoms
such as changes in eating or sleeping patterns, fatigue, difficulty concentrating, indecision, thoughts of death or suicide, or feelings of worthlessness, helplessness, or hopelessness (16). It is important to note that these symptoms must
represent a change from the individual’s usual self and cause
clinically significant distress or impairment. In addition,
they cannot be attributable to bereavement or another disorder, including a substance-induced condition or a general
medical condition. In some individuals, hallucinations or
delusions may occur in the context of a major depressive episode, in which case the episode would be specified as “Severe With Psychotic Features.” When psychotic features
are present, they may either be mood congruent (typically
involving themes such as guilt, punishment, personal inadequacy, or disease) or mood incongruent. Although not a
part of the DSM-IV-TR criteria, anxiety and somatic symptoms (particularly muscular, respiratory, and genitourinary)
can also be seen in the context of major depressive disorder
(975). Episodes of major depression may also be distinguishable by their longitudinal course (e.g., chronic if
symptoms are present for at least 2 years, postpartum onset
if symptoms occur within 4 weeks postpartum, seasonal pattern if the timing of episodes is regularly associated with a
specific time of year) (16) and characteristic subsets of episode features (Table 12).
B. EPIDEMIOLOGY
Information on the current prevalence of major depressive disorder comes from two large community surveys,
the National Comorbidity Survey Replication (NCS-R)
study (976) and the National Epidemiologic Survey of Alcoholism and Related Conditions (NESARC) (655). In
the NCS-R, the lifetime prevalence of major depressive
disorder among the 9,090 adult participants was 16.2%,
with a 12-month prevalence of 6.6%. The NESARC, which
included more than 43,000 adults found slightly lower
prevalence rates than the NCS-R (13.25% lifetime and
5.28% 12-month), perhaps because the sample included
previously omitted groups of individuals with lower prevalence rates (655). A number of sociodemographic factors
appears to be associated with an increased prevalence of
major depressive disorder, including female sex, being
middle-aged, being never or previously married, having a
low income, being unemployed, or being disabled (655,
976), In the NESARC, being Native American increased
risk relative to being Caucasian, whereas being Asian,
Hispanic, or black decreased risk (655).
The impact of major depressive disorders on individuals and their families is substantial. Virtually all individuals
in the NCS-R who had a major depressive episode in the
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preceding 12-month period experienced significant levels
of symptom severity as assessed by an independent rating
scale (976). For more than 50% of individuals, symptoms
were rated at severe or very severe (976) and were associated with substantial role impairment (977).
Major depressive disorder rarely occurs in isolation;
anxiety disorders, substance use disorders, personality disorders, and impulse control disorders commonly co-occur
with major depressive disorder in community samples (655,
976) as well as in individuals in psychiatric treatment (978).
In the NCS-R, major depressive disorder was found to cooccur with at least one other DSM-IV disorder in twothirds of those surveyed (976), but from a temporal standpoint major depressive disorder was the primary diagnosis
in only about 12% of these individuals (976). In contrast, in
a study of patients in psychiatric treatment in the United
States, 84% of major depressive disorder patients had at
least one co-occurring condition: 61% had a co-occurring
Axis I condition, 30% a co-occurring Axis II condition, and
58% a co-occurring Axis III condition (978). Anxiety disorders were the most common co-occurring disorder in the
prior 12 months in both the NCS-R (57.5% of the sample)
(976) and the NESARC (36.1% of the sample) (655). Of
the anxiety disorders, the greatest association was seen with
generalized anxiety disorder and the weakest association
with specific phobia (655). Substance use disorders in the
preceding 12-month period were less common in the
NCS-R (8.5%) (976) than in the NESARC, in which
14.1% of the individuals with major depressive disorder
had an alcohol use disorder, 26.0% had nicotine dependence, and 4.6% had another substance use disorder (655).
Personality disorders were present in 37.9% of individuals
with major depressive disorder in the NESARC (655). Obsessive-compulsive, paranoid, schizoid, and avoidant personality disorders were most common among subjects with
major depressive disorder; avoidant, dependent, paranoid,
and schizoid personality disorders had greater odds ratios
for association with major depressive disorder than other
personality disorders (655).
Treatment of major depressive disorder does not always
occur and may be delayed. The average time to treatment
in the NESARC was approximately 3 years, and only about
60% of the sample with major depressive disorder received
treatment (655). The NCS-R also evaluated history and
adequacy of treatment for major depressive disorder (976).
Of respondents who reported having had a major depressive episode in the last year, just more than one-half had received treatment but less than one-half of these individuals
(about one-fifth of the total) received adequate treatment
(976). These findings highlight the need for changes in the
delivery of mental health services to enhance the timeliness
and quality of care for major depressive disorder.
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
TABLE 11.
79
DSM-IV-TR Criteria for Major Depressive Episode and Major Depressive Disorder
Diagnosis
Criterion/Symptom Description
Major depressive episode
A. At least five of the following symptoms have been present during the same
2-week period and represent a change from previous functioning; at least one
of the symptoms is either 1) depressed mood or 2) loss of interest or pleasure
(do not include symptoms that are clearly due to general medical condition or
mood-incongruent delusions or hallucinations).
1.
2.
3.
4.
5.
6.
7.
8.
9.
Depressed mood most of the day, nearly every day, as indicated either by
subjective report (e.g., feels sad or empty) or observation made by others
(e.g., appears tearful)
Markedly diminished interest or pleasure in all, or almost all, activities
most of the day, nearly every day (as indicated either by subjective account
or observation made by others)
Significant weight loss when not dieting or weight gain (e.g., a change of
more than 5% of body weight in a month), or decrease or increase in
appetite nearly every day
Insomnia or hypersomnia nearly every day
Psychomotor agitation or retardation nearly every day (observable by
others, not merely subjective feelings of restlessness or being slowed down)
Fatigue or loss of energy nearly every day
Feelings of worthlessness or excessive or inappropriate guilt (which may be
delusional) nearly every day (not merely self-reproach or guilt about being
sick)
Diminished ability to think or concentrate, or indecisiveness, nearly every
day (either by subjective account or as observed by others)
Recurrent thoughts of death (not just fear of dying), recurrent suicidal
ideation without a specific plan, or a suicide attempt or specific plan for
committing suicide
B. The symptoms do not meet criteria for a mixed episode.
C. The symptoms cause clinically significant distress or impairment in social,
occupational, or other important areas of functioning.
D. The symptoms are not due to the direct physiological effects of a substance
(e.g., a drug of abuse, a medication) or a general medical condition (e.g.,
hypothyroidism).
E. The symptoms are not better accounted for by bereavement, i.e., after the loss
of a loved one, the symptoms persist for longer than 2 months or are
characterized by marked functional impairment, morbid preoccupation with
worthlessness, suicidal ideation, psychotic symptoms, or psychomotor
retardation.
Major depressive disorder,
single episode
A. Presence of a single major depressive episode.
B. The major depressive episode is not better accounted for by schizoaffective
disorder and is not superimposed on schizophrenia, schizophreniform disorder,
delusional disorder, or psychotic disorder not otherwise specified.
C. There has never been a manic episode, a mixed episode, or a hypomanic
episode.
(continued)
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80
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TABLE 11.
DSM-IV-TR Criteria for Major Depressive Episode and Major Depressive Disorder (continued)
Diagnosis
Criterion/Symptom Description
Major depressive disorder,
recurrent
A. Presence of two or more major depressive episodes (each separated by at least
2 months in which criteria are not met for a major depressive episode).
B. The major depressive episodes are not better accounted for by schizoaffective
disorder and are not superimposed on schizophrenia, schizophreniform
disorder, delusional disorder, or psychotic disorder not otherwise specified.
C. There has never been a manic episode, a mixed episode, or a hypomanic
episode
Source. Reprinted from Diagnostic and Statistical Manual of Mental Disorders, 4th Edition, Text Revision. Washington, DC, American
Psychiatric Association, 2000. Copyright © 2000, American Psychiatric Association.
TABLE 12.
Selected DSM-IV-TR Major Depressive Episode Specifiers
Criteria for Melancholic Features Specifier
A. Either of the following, occurring during the most severe period of the current episode:
1.
loss of pleasure in all, or almost all, activities
2.
lack of reactivity to usually pleasurable stimuli (does not feel much better, even temporarily, when something
good happens)
B. Three (or more) of the following:
1.
distinct quality of depressed mood (i.e., the depressed mood is experienced as distinctly different from the
kind of feeling experienced after the death of a loved one)
2.
depression regularly worse in the morning
3.
early morning awakening (at least 2 hours before usual time of awakening)
4.
marked psychomotor retardation or agitation
5.
significant anorexia or weight loss
6.
excessive or inappropriate guilt
Criteria for Atypical Features Specifier
A. Mood reactivity (i.e., mood brightens in response to actual or potential positive events)
B. Two (or more) of the following features:
1.
significant weight gain or increase in appetite
2.
hypersomnia
3.
leaden paralysis (i.e., heavy, leaden feelings in arms or legs)
4.
long-standing pattern of interpersonal rejection sensitivity (not limited to episodes of mood disturbance) that
results in significant social or occupational impairment
C. Criteria are not met for With Melancholic Features or With Catatonic Features during the same episode.
Criteria for Catatonic Features Specifier
The clinical picture is dominated by at least two of the following:
1.
motoric immobility as evidenced by catalepsy (including waxy flexibility) or stupor
2.
excessive motor activity (that is apparently purposeless and not influenced by external stimuli)
3.
extreme negativism (an apparently motiveless resistance to all instructions or maintenance of a rigid posture
against attempts to be moved) or mutism
4.
peculiarities of voluntary movement as evidenced by posturing (voluntary assumption of inappropriate or
bizarre postures), stereotyped movements, prominent mannerisms, or prominent grimacing
5.
echolalia or echopraxia
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
C. NATURAL HISTORY AND COURSE
The age at onset of major depressive disorder varies widely,
although the average age at onset is the late 20s. Although
the onset of the first episode is rarely before puberty, the disorder may begin at any age (655, 976). Symptoms of major
depressive disorder typically develop over days to weeks.
Prodromal symptoms, including generalized anxiety, panic
attacks, phobias, or depressive symptoms that do not meet
the diagnostic threshold may occur over the preceding several months. In some individuals, however, major depressive
disorder may develop suddenly, as in the wake of severe psychosocial stress. The duration of a major depressive episode
also varies. The mean duration of a major depressive episode
was 16 weeks in the NCS-R (976), with a median duration for
the longest depressive episode of 24.3 weeks in the NESARC
(655). In treated patients, the median time to recovery from a
major depressive episode is approximately 20 weeks (979).
Untreated, episodes typically last 6 months or longer. Some
patients with major depressive disorder eventually have a
manic or hypomanic episode, and they will then receive a
new diagnosis of bipolar I disorder or bipolar II disorder.
1. Recurrence
Major depressive disorder is unremitting in 15% of patients
and recurrent in 35%. About half of those with a first-onset episode recover and have no further episodes (502).
After three episodes, the risk of recurrence approaches
100% in the absence of prophylactic treatment. Individuals with major depressive disorder superimposed on dysthymic disorder carry a greater risk for having recurrent
episodes of major depressive disorder than those without
dysthymic disorder (410). When major depressive disorder is recurrent, its course varies. Some people have episodes separated by many years of normal functioning,
others have clusters of episodes, and still others have increasingly frequent episodes as they age.
2. Interepisode status
Functioning usually returns to the premorbid level between
V.
81
episodes. However, 20%–35% of patients have persistent
residual symptoms and social or occupational impairment.
Patients who continue to have depressive symptoms but fall
below the diagnostic threshold for major depressive disorder are considered to be in partial remission. Residual depressive symptoms increase the risk of relapse. Anxiety and
somatic symptoms are particularly prominent residual
symptoms of major depressive disorder (980).
3. Complications and prognosis
Major depressive disorder adversely affects the patient and
others. The most serious complication of a major depressive episode is suicide (including suicide/homicide). Major
depressive disorder is also associated with significant medical comorbidity and complicates recovery from other
medical illnesses, such as myocardial infarction (see Section
III.C.1). Beyond its impact on the patient alone, major depressive disorder also affects the patient’s marital, parental,
social, and vocational functioning (981). The disorder, especially when recurrent or chronic, may distress other individuals in the patient’s social network, e.g., children,
spouse, and significant others. If the patient is a parent, the
disorder may affect his or her ability to fulfill parental role
expectations (982) and increase the likelihood of children
becoming depressed as well (see Section III.B.5). Major depressive episodes are associated with occupational dysfunction, including unemployment, absenteeism, and decreased
work productivity (977, 983). In fact, in terms of the level of
disability for the population as a whole, major depressive
disorder was second only to chronic back and neck pain in
disability days per year (977).
The prognosis for major depressive disorder depends on
many factors, such as treatment status, availability of supports, chronicity of symptoms, and the presence of co-occurring medical and psychiatric conditions. With treatment,
however, the prognosis is generally good (984). Most patients will respond to acute treatment, and continuation and
maintenance treatment with acutely active treatments has
been shown to lower the risk and severity of relapse.
REVIEW AND SYNTHESIS OF AVAILABLE EVIDENCE
Translating the product of science into a decision about a
single human patient raises the concept of epistemology:
how we know what we think we know and how certain we
can be about that knowledge. Like all guidelines, this one
is an attempt to distill clinical research into recommendations that will be clinically applicable to the unique indi-
vidual who presents for treatment. Science can never
provide all of the answers that a doctor or patient wishes
and, at times, the knowledge base may consist primarily of
accumulated wisdom from clinical experience. In addition, every scientific protocol reflects a series of compromises, and each compromise may restrict internal and/or
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82
external validity, as described later in this section. No one
study, with its inevitable limits, can reveal “truth.” The
wise scientist—and physician—demands replication. When
multiple trials, with different methods, come to similar
conclusions, the clinician can be reasonably confident in
the results.
Many aspects of the design of research studies can influence the interpretation of the data and their implication for
clinical practice. When translating efficacy evidence to
clinical practice, it is important to assess the adequacy of
the sample size (given modest effect sizes of antidepressant treatments), the nature and validity of the control
condition, the length of the treatment trial, the nature of
the participant population, the type and reliability of the
outcome measure, and publication bias (in favor of positive trials) (74, 985, 986).
Some issues also exist that are specific to pharmacotherapy trials. First, it is important to consider whether
and what type of comparison group was used (e.g., placebo or active agent). In trials of antidepressant medication treatments, high placebo response rates could make
detection of true treatment effects difficult in wellcontrolled trials, as well as explain observed treatment effects in trials with less robust controls. It is also important
to consider whether trials were blinded and, if so, whether
medication side effects could reveal the identity of active
agents. Issues related to the outcomes measured in trials
are important as well. A variety of different outcome measures are employed, and a report of “efficacy” could refer
to symptom reduction (e.g., reduction in the frequency or
severity of major depressive disorder symptoms), response (e.g., reduction in major depressive disorder symptoms below a threshold), or prevention of relapse. Despite
the fact that a 2006 American College of Neuropsychopharmacology task force report (408) emphasized the need
to aim for remission as a primary goal, studies may not be
designed and powered statistically to assess remission as a
primary outcome. Until recently most research studies
have reported response rates, often defined as a reduction
by 50% in the measured severity of depression. In addition, data often come from short-term (6- to 12-week)
efficacy trials that cannot show whether treatments are effective over the medium- and long-term. There has also
been recent concern that the apparent effect size of antidepressants has been exaggerated, due to the lack of reporting or selective publication of negative clinical trial
data (74, 75). A national database of clinical trial data
(http://clinicaltrials.gov/) is being expanded in an effort to
make these data available and transparent (987). However,
most meta-analyses were published prior to this initiative,
and previously conducted studies will not be subject to the
provisions of recent regulations (988).
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Evaluating the efficacy of psychotherapeutic approaches for major depressive disorder can also be challenging. Although there have been a number of welldesigned trials of CBT and IPT in large samples, for some
other types of psychotherapy, few or no clinical trials have
been conducted. In studies evaluating psychotherapy
against a variety of control conditions such as waiting lists,
other forms of psychotherapy, medications, placebos, or a
no-control group, it is difficult to make comparisons of the
observed treatment effect sizes among trials. Some trials
have not examined the effects of psychotherapy exclusively
among patients with major depressive disorder and may
not have specifically assessed improvement in major depressive disorder as an outcome. In other trials, the nature
of the psychotherapeutic intervention has been insufficiently described, making it difficult to apply the study
findings to psychotherapeutic approaches used in practice.
In evaluating the impact of a particular intervention,
several statistical concepts are helpful to understand. If one
starts with the assumption that the treatment group and the
control group are equivalent (i.e., no effect of treatment),
the p value indicates the probability that the treatment
group will show an outcome that is equal to or more extreme
than the observed treatment outcome (989). Although specific values of p (e.g., 0.05) are commonly considered to be
statistically significant, the p value does not address the
possibility, known as a type II error, that the treatment
group and control group will have similar outcomes even
though the treatment is actually effective. This possibility
can be reduced, to some extent, by using sufficiently sized
research samples, which should be calculated as part of the
study design (i.e., power analysis). Because these concepts
are difficult to grasp and provide limited information about
the clinical importance of an observed impact of treatment,
several other measures are often used. One approach to indicating the benefit of a treatment relative to a control condition is the number needed to treat (NNT), which is the
number of individuals who would have to be treated to prevent one negative outcome (or benefit one patient) (990).
When applied to adverse effects, such a measure is termed
the number needed to harm (NNH). The effect size is a
measure of the magnitude of the difference between the
treatment group and the control group, which also considers the variability of the measurements. When the statistic
Cohen’s d is used to measure the size of a treatment effect,
a general rule-of-thumb is that d=0.2 represents a small effect, d=0.5 represents a medium effect, and d=0.8 (or
greater) represents a large effect of the intervention (991).
In addition to being used in describing the results of individual studies, effect sizes are also used in comparing and
synthesizing the results of multiple clinical trials through
meta-analyses.
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
A. ACUTE PHASE SOMATIC TREATMENTS
1. Antidepressant medications
a.
Selective serotonin reuptake inhibitors
Many studies and meta-analyses have compared SSRIs
among themselves as well as with other classes of antidepressants. Differences in efficacy and tolerability between SSRIs and TCAs, assessed through a meta-analysis
of 102 studies (85), found no overall difference in efficacy
between TCAs and SSRIs. However, TCAs appeared
more efficacious in inpatients (p=0.012), and amitriptyline was more effective than SSRI comparators (p=0.012),
although publication bias could not be excluded. By contrast, SSRIs as a class (p<0.01) and, more specifically, paroxetine (p=0.001), fluoxetine (p<0.01), sertraline (p<0.05),
and citalopram (p<0.01) had a significantly lower rate of
dropouts for side effects. Other meta-analyses have compared the SSRIs among themselves and with other newer
antidepressant agents. Cipriani and colleagues (96) performed a multiple-treatments meta-analysis, which encompassed 117 randomized controlled trials and 25,928 subjects.
Incorporating efficacy and treatment discontinuation, they
found the greatest degree of overall acceptability with
escitalopram and sertraline, with greatest efficacy for
mirtazapine, escitalopram, venlafaxine, and sertraline as
compared with duloxetine, fluoxetine, fluvoxamine, paroxetine, and reboxetine. Gartlehner and colleagues (95)
also compared the benefits and side effects of secondgeneration antidepressants including SSRIs using 6 goodor fair-quality systematic reviews or meta-analyses and
155 good- or fair-quality double-blind, placebo-controlled, or head-to-head randomized controlled trials of at
least 6 weeks' duration to assess efficacy and 35 observational
studies with at least 100 participants and follow-up of at
least 12 weeks to assess harms. Although the side effect
profiles and onset of action differed among the antidepressants, no differences in efficacy or effectiveness were
found.
A systematic review of 28 randomized studies (89) showed
that, even in anxious depression, SSRIs (fluoxetine, paroxetine, citalopram, sertraline, and escitalopram) are comparable in efficacy to other antidepressant medications
(bupropion, amitriptyline, mirtazapine, imipramine, nefazodone, and venlafaxine), both in depression and anxiety
parameters. When compared with venlafaxine, fluoxetine
was less effective both in depression and anxiety scores,
while paroxetine was less effective in anxiety scores only.
No differences were found between venlafaxine and the
other SSRIs.
A Cochrane meta-analysis (84) that included 132 randomized studies (almost all double blind) did not find sig-
83
nificant differences in fluoxetine efficacy versus TCAs.
When fluoxetine was compared with newer antidepressants, venlafaxine was superior, and within the class of
SSRIs, sertraline was significantly superior. However, fluoxetine was significantly better tolerated than TCAs as a
class and, more specifically, was better tolerated than amitriptyline, clomipramine, desipramine, and imipramine; no
differences were noted in comparison with all of the other
medications. Similar meta-analyses compared sertraline
(126) and escitalopram (992) to other antidepressive agents.
Although differences were small, there was a trend for sertraline to be more acceptable and efficacious than comparator antidepressants, including TCAs, SSRIs, and several
newer antidepressants (126). Escitalopram was found to be
more efficacious than citalopram and fluoxetine in terms of
response and remission of depressive symptoms and was associated with lower rates of treatment discontinuation than
subjects receiving duloxetine (992).
Another meta-analysis of 21 studies (98) compared efficacy and tolerability of each SSRI (except escitalopram)
against the SSRI class overall and showed no difference in
efficacy among the drugs. Rates of dropout due to side
effects were significantly lower in patients treated with
sertraline (p<0.05) and significantly higher in patients
treated with fluvoxamine (p<0.01), although the dropout
rate in fluvoxamine-treated patients appeared to vary with
medication dose. In this meta-analysis, side effects and
discontinuation reactions were observed more often with
paroxetine than with other SSRIs. Interaction with other
drugs was higher with fluoxetine, fluvoxamine, and paroxetine than with sertraline and citalopram, although citalopram was overrepresented in deaths due to overdose.
A systematic review based on 18 randomized, doubleblind trials (94), which compared escitalopram with either
citalopram, venlafaxine, paroxetine, sertraline, or bupropion, found no differences in efficacy between escitalopram
and the other medications (except for the comparison
with citalopram, which showed a significant difference in
two of four studies). Rates of study withdrawal due to side
effects were lower with escitalopram than with venlafaxine (p<0.05) or paroxetine (p<0.05).
Another meta-analysis of 32 randomized clinical trials
studied the efficacy and tolerability of antidepressants in
people older than age 55 years (704). This study found
that there was no difference in efficacy between TCAs and
SSRIs, but SSRIs were better tolerated. Compared with
patients who were taking TCAs, patients who were taking
SSRIs were less likely to withdraw from the study overall
or because of side effects, in particular. The qualitative
analysis of side effects showed a small increase in gastrointestinal and neuropsychiatric side effects associated
with TCAs.
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Overall, the findings of multiple randomized trials and
meta-analyses indicate comparable efficacies for SSRIs
relative to TCAs, although some data suggest greater efficacy for TCAs in inpatient samples. Selective serotonin
reuptake inhibitors also appear to have comparable efficacy to other non-TCA antidepressants, although venlafaxine shows superior efficacy in some studies, and
comparisons of SSRIs and MAOIs have not been done. In
terms of tolerability, SSRIs show consistently fewer dropouts in clinical trials than TCAs, and side effects are also
reported less often with SSRIs. There also do not seem to
be significant differences in efficacy among the SSRIs.
Fluvoxamine appears to have more side effects and more
problems with drug interactions than the other SSRIs;
drug interactions are also more problematic with fluoxetine and paroxetine than with citalopram, escitalopram, or
sertraline.
b. Serotonin norepinephrine reuptake inhibitors
The efficacy of venlafaxine, desvenlafaxine, and duloxetine,
which are classified as SNRIs, and mirtazapine, which
(although not an SNRI) also enhances both serotonin and
norepinephrine neurotransmission, has been demonstrated in placebo-controlled studies of depressed patients
(101, 102, 105, 113, 993, 994, 995). A number of studies
have contrasted these “dual-action” antidepressants with
the SSRIs. Although most individual studies have not
found statistically significant differences (see, for example, references 226 and 421), meta-analyses of controlled
studies of venlafaxine (101, 104, 996, 997), duloxetine
(102), and mirtazapine (113) using SSRIs as comparators
have generally documented small (i.e., 4%–10%) albeit
reliable differences in the likelihood of response or remission favoring the dual-action drugs. Papakostas et al.
(995) similarly found an average difference of 4% in response/remission rates in a meta-analysis of a broader
grouping of antidepressant drugs that affect norepinephrine and serotonin. These average effects are generally
below the magnitude of difference that is widely considered to be clinically significant. It is possible that a small
average difference in an overall pool of patients may obscure larger and more meaningful differences among
selected subgroups of depressed patients (e.g., more severely depressed patients [102], inpatients [561], or postmenopausal women [998]), but this suggestion has yet to
be confirmed by analyses of larger data sets. At present,
the efficacy of desvenlafaxine has only been established
versus placebo (993, 994); there are not yet any published
studies assessing its benefits relative to other antidepressants. Nevertheless, as the principal active metabolite
of venlafaxine, it is likely to have a comparable efficacy
profile.
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Perahia et al. (999) conducted a randomized controlled
trial of duloxetine versus paroxetine and placebo in an
outpatient setting in patients who met the criteria for
major depressive disorder. After 8 weeks, duloxetine at
80 mg/day (N=93) and at 120 mg/day (N=103) was found
to be superior to placebo (N=99). However, paroxetine
was not superior to placebo in this study. Perahia et al. also
conducted a relapse prevention study (1000), in which patients were randomly assigned to receive duloxetine or
placebo for 26 weeks after a 12-week open-label treatment phase. The 136 patients who received duloxetine
had a relapse rate of 23%, compared with the 39% relapse
rate among the 142 patients who received placebo
(p≤0.005). A large cohort study by Raskin et al. (1001)
followed 1,279 patients in 52 treatment centers taking
80–120 mg/day of duloxetine over 52 weeks. Patients
were assessed by multiple instruments at 6, 28, and 52
weeks. At 6 weeks, 50.8% achieved a score of <8 on the
HAM-D. The rate of response increased to 75.6% at week
28 and 81.7% at week 52, with no safety concerns identified in the course of the study.
Venlafaxine extended release (XR) has also been extensively studied. Rudolph and Feiger (1002) conducted
an 8-week outpatient trial of venlafaxine XR compared
with fluoxetine and placebo. In this trial, 100 patients received venlafaxine XR (75–225 mg/day), 193 received fluoxetine (20–60 mg/day), and 98 received placebo.
Remission rates, determined by an HRSD score of <8,
were 37% in the venlafaxine XR arm, 22% in the fluoxetine
arm, and 18% in the placebo arm. Sauer et al. (1003)
compared 76 patients who received venlafaxine XR (75–
150 mg/day) with 75 patients who received amitriptyline
(75–150 mg/day). Venlafaxine XR yielded response rates
of 39.5%, compared with 41.7% for amitriptyline. SaizRuiz et al. (1004) followed 59 patients receiving venlafaxine over 6 months. Seventy percent of these patients completed the study, and the response rate, determined by a
50% reduction in the HRSD score, was 81%. In another
cohort study, Mitchell et al. (1005) found response rates at
8 weeks to be 52.6%, measured by the MADRS, among
312 patients with treatment-resistant illness taking venlafaxine in an open-label trial. Response rates at 10 months
as measured by the MADRS increased to 73% in 149 patients who continued treatment in an extension phase of
the study (1006).
Fewer studies have been conducted with desvenlafaxine; however, meta-analysis shows that it also is efficacious
in the acute treatment of major depressive disorder (99).
In the nine randomized, double-blind, placebo-controlled 8-week long trials with desvenlafaxine, there were
1,342 subjects in fixed dose study arms (50, 100, 200, or
400 mg/day), 463 subjects in flexible dose study arms
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
(100–400 mg/day), and 1,108 subjects in placebo study
arms. Desvenlafaxine showed greater efficacy than placebo in rates of response as well as remission, with no
greater benefit (and greater discontinuation rates) at doses
greater than 50 mg daily. Overall rates of treatment discontinuation due to adverse effects were 3% for placebo
and 12% for desvenlafaxine (168). Treatment emergent
adverse effects included transient nausea and erectile dysfunction in men. Mean blood pressure was statistically increased in the desvenlafaxine group, but this change was
clinically significant in only 2% of desvenlafaxine subjects, compared with 1% of the placebo group.
c.
Other antidepressant medications
1. Bupropion
Meta-analyses of controlled trials have shown that bupropion is superior to placebo and is generally comparable in
efficacy to both TCAs and SSRIs (105, 169, 1007). All
three formulations of bupropion are superior to placebo
(106), and early studies with the immediate-release formulation found it to be generally comparable in efficacy
to the TCAs (105, 1008–1011). The newer sustainedrelease and extended-release formulations have been primarily compared with the SSRIs, and meta-analyses have
established comparable efficacy (169, 1012).
Several studies have compared bupropion sustained release (SR) to SSRIs and placebo. A randomized controlled
trial by Croft et al. (1013) compared bupropion SR to sertraline and placebo over 8 weeks of treatment and found
both drugs to have efficacy superior to placebo. Bupropion SR had a lower rate of sexual dysfunction than sertraline. These findings were confirmed in a 16-week study
that again compared bupropion SR with sertraline and
placebo (1014). Another 8-week study found bupropion
SR, but not sertraline, to be superior to placebo and again
documented lower rates of sexual dysfunction with bupropion SR than sertraline (1015). Similar results were found
when bupropion SR was compared with other SSRIs. One
study comparing bupropion SR with paroxetine found
equivalent efficacy (1016). In another trial, with approximately 150 patients in each arm, bupropion had similar
efficacy to fluoxetine with a significantly lower burden of
side effects (1017). Lower rates of sexual dysfunction have
also been found with bupropion compared with sertraline
(1013–1015) or paroxetine (1016). A survey of 6,297 patients in primary care settings found the incidence of sexual
dysfunction with bupropion to be 22%–25%. This incidence was comparable to the incidence with nefazodone
(28%) but lower than that with SSRIs and venlafaxine
(36%–43%) (1018). Several small studies have examined
whether bupropion might serve as a potential treatment
85
for SSRI-induced sexual side effects, with varying results
(132, 1019, 1020).
Bupropion has also been studied as a treatment for anxiety associated with major depressive disorder. In one
large trial, patients were randomly assigned to receive bupropion SR (N=234), sertraline (N=225), or placebo
(N=233). Patients treated with bupropion SR or sertraline
experienced significantly greater relief from anxiety symptoms than those who received placebo. Compared with
sertraline, bupropion appeared to be associated with similar relief of anxiety in patients with major depressive disorder (1021).
Bupropion has also been shown to reduce the risk of relapse following successful antidepressant treatment with
bupropion. In a 44-week double-blind trial of bupropion
responders (1022), patients were randomly assigned to continue taking bupropion or change to placebo. Continued
treatment with bupropion after acute phase response reduced the risk of relapse, compared with placebo, with few
differences in side effects reported between the two groups.
2. Mirtazapine
The efficacy of mirtazapine has been established in placebo-controlled studies (1023, 1024), two individual studies versus venlafaxine (1025, 1026), and in meta-analyses
of studies comparing it to TCAs (1027–1029) and SSRIs
(1030). Quitkin et al. (1030) analyzed three studies comparing patients with major depressive disorder treated
with mirtazapine (N=289) to patients treated with fluoxetine or paroxetine (N=285). Although mirtazapine and
SSRIs had similar efficacy over 6–8 weeks, a greater proportion of patients had onset of therapeutic benefit at
week 1 with mirtazapine as compared with an SSRI (13%
versus 6%). In a meta-analysis by Watanabe et al. (1031),
mirtazapine was superior to SSRIs in response and remission rates at 2 weeks (12 trials), although it was comparable to SSRIs at the end of treatment (6–12 weeks). In a
subgroup analysis, mirtazapine produced greater response
than paroxetine (three trials) and venlafaxine (two trials).
At 2 weeks as well as at the end of 6–12 weeks’ treatment
(8 trials used to obtain outcomes), mirtazapine had comparable efficacy to TCAs. A meta-analysis of six studies
(1027) found mirtazapine to have comparable efficacy to
amitriptyline over 6–8 weeks, with both drugs showing
superiority to placebo.
Several randomized controlled trials have compared
mirtazapine to SSRIs. Benkert et al. (1032) randomly assigned patients with major depressive disorder to treatment with mirtazapine (N=127) or paroxetine (N=123)
over 6 weeks, and Wade et al. (1033) randomly assigned
197 primary care patients with HAM-D scores of at
least 18 to mirtazapine (N=99) or paroxetine (N=98) over
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86
24 weeks of treatment. In both studies, the treatments had
equal efficacy at study endpoint, but mirtazapine demonstrated a different profile of side effects. Another trial randomly assigned elderly depressed patients (at least age
65 years) to mirtazapine (N=126) or paroxetine (N=120)
over 8 weeks (1034). Compared with paroxetine, mirtazapine showed a greater benefit at day 14, had less attrition
for side effects, and was significantly more effective in improving sleep. It was also more effective in reducing
HAM-D scores by the study endpoint, although response
and remission rates were not significantly different. Two
randomized trials, one 8 weeks long (N=299) (1035) and
the other a 6-week study (N=132) in Chinese patients,
have compared treatment with mirtazapine to fluoxetine
and found no differences in overall efficacy, although the
onset of improvement and side effect profiles differed as
with paroxetine. A similar pattern of outcomes was also
observed when mirtazapine was compared with citalopram
(N=270) in an 8-week trial (1036) and when an oral disintegrating form of mirtazapine was compared with sertraline (N=345) in another 8-week trial (1037).
Mirtazapine has also been compared with venlafaxine
(both immediate release [IR] and extended release [XR]
forms) in randomized controlled trials. In an 8-week trial,
Guelfi et al. (1025) followed patients with major depressive disorder (HAM-D scores of at least 25) receiving mirtazapine (N=78) and venlafaxine IR (N=79). Mirtazapine
and venlafaxine did not differ significantly in depression
outcomes, although sleep was better with mirtazapine,
and significantly more patients taking venlafaxine IR (15%)
dropped out due to side effects, compared with patients
taking mirtazapine (5%). A similar 8-week trial (1026)
found no significant differences in final outcome or tolerability between venlafaxine XR and mirtazapine, although
mirtazapine showed greater benefit during the first 15 days
of therapy.
Patients with major depressive disorder who were not
responsive or who were intolerant of two prior treatments
with antidepressants were randomly assigned to treatment with mirtazapine (N=114) or nortriptyline (N=121)
for up to 12 weeks as part of the STAR*D trial (471). Remission rates were 12% for mirtazapine and 20% for nortriptyline. There were no significant differences in any
outcome measure, and the medications were comparably
tolerated. Neither mirtazapine nor nortriptyline was particularly effective as monotherapy for patients who had
not benefited from two consecutive treatment trials.
Mirtazapine has been shown to decrease rates of relapse following acute phase treatment. Thase et al. (1038)
compared 78 patients who received mirtazapine to 78 patients who received placebo over 9 months following an
8- to 12-week treatment with an antidepressant. Patients
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taking mirtazapine had about a 50% reduction in relapse
rates. However, patients taking mirtazapine gained 1.4 kg
more weight than those taking placebo across the 9 months
of continuation phase therapy.
3. Nefazodone and trazodone
The efficacy of nefazodone has been established in placebo-controlled trials, with efficacy comparable to both
TCAs and SSRIs (105, 1039–1042); however, its recent
use has been limited after case reports suggested a risk of
rare but potentially fatal hepatotoxicity (180). While an
early review of trazodone (114) concluded that trazodone
is as effective as TCAs in the treatment of depression,
other investigators have found trazodone to be less effective than other antidepressant medications (115, 1043–
1045), a conclusion supported by the results of at least one
meta-analysis (93). In a review of 18 studies from 1980
through 2003, Mendelson (173) found that trazodone, when
compared with various control groups, did improve sleep.
However, it was also associated with significant side effects, and tolerance may develop with prolonged use.
d.
Tricyclic antidepressants
Since the first trial in which a tricyclic compound (imipramine) was shown to improve major depressive disorder
symptoms (1046), hundreds of subsequent randomized
controlled trials have demonstrated the efficacy of this antidepressant class as a treatment for major depressive disorder (105). Several reviews of this early literature
suggested that approximately 50%–75% of patients with
major depressive disorder treated with tricyclic and related antidepressant medications respond, compared with
25%–33% of patients who receive placebo (487, 1047–
1049). The efficacy of individual agents and subclasses of
tricyclics (e.g., secondary amines or tertiary amines) appears to be comparable, although amitriptyline may possess a slightly stronger effect across all studies (1050), and
the tertiary amine tricyclics (amitriptyline, clomipramine,
and imipramine) may have a stronger antidepressant effect than the secondary amine tricyclics and maprotiline
in studies of hospitalized depressed patients (117).
The meta-analysis of Barbui et al. (1050) reviewed 181
randomized controlled trials of amitriptyline, generally of
6–8 weeks’ duration, in inpatient and outpatient settings.
Amitriptyline was found to be superior to SSRIs in studies
of inpatients, but there was no difference in efficacy in
outpatients. Selective serotonin reuptake inhibitors were
better tolerated. Arroll et al. (1051) compared TCAs with
SSRIs in a meta-analysis of 15 randomized controlled trials in primary care settings. Both TCAs and SSRIs were
effective, but tolerability comparisons across studies favored SSRIs. Wohlfarth et al. (1052) reviewed 30 random-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
ized controlled trials conducted between 1979 and 1991,
with a combined sample size of 1,555 men and 2,331 women.
Tricyclic antidepressants were more effective than placebo across age and gender groups.
Several trials have compared TCAs against interpersonal therapy and CBT and against the combination of
TCAs and IPT or CBT. Reynolds et al. (1053) followed
80 patients who were at least age 50 years and had a bereavement-related depression in a 16-week factorial design
trial in which patients received IPT or case management
and nortriptyline or placebo. Nortriptyline (with or without IPT) was more effective than placebo (with or without
IPT). Patients receiving combined nortriptyline and IPT
had the highest study completion rate. Interpersonal psychotherapy alone (i.e., IPT plus placebo) was not found
to be an effective treatment for bereavement-related major depressive disorder. However, in a continuation trial
(N=107) over 24 months (315), combination therapy was
found to be more effective than monotherapy in patients
age 70 years or older. All patients had been first stabilized
on combination nortriptyline and IPT before entering
the continuation phase. In a 16-week randomized controlled trial among 102 elderly patients with major depressive disorder, Thompson et al. (1054) found that
combined treatment with CBT and nortriptyline was superior to CBT alone, which was superior to nortriptyline
alone. Combined treatment was particularly effective in
patients with severe depression, as measured by HAM-D
scores.
For patients with major depressive disorder who received ECT following a prior nonresponse to treatment
with an antidepressant, van den Broek (1055) found that
12 patients randomly assigned to receive imipramine
(200–300 ng/mL plasma level) had a greater improvement
in all measures in preventing relapse than the 15 patients
randomly assigned to receive placebo.
Results of some investigations have suggested that TCAs
are particularly effective for patients with more severe
symptoms of major depressive disorder (1056–1060), as well
as for patients with melancholia (562, 1061–1063). Superior
efficacy for TCAs, compared with SSRIs, has been documented in meta-analyses of inpatient studies (117).
e. Monoamine oxidase inhibitors
Monoamine oxidase inhibitors have also been shown in
multiple trials to be effective treatments for major depressive disorder. Although some earlier comparisons employing lower doses of MAOIs found TCAs to be superior,
MAOIs are now considered to have comparable efficacy
to TCAs for most patients with major depressive disorder
(119, 120, 1064–1067). Results of several investigations
suggest that MAOIs may be particularly effective in treat-
87
ing subgroups of patients with major depressive disorder
with atypical features such as reactive moods, reversed
neurovegetative symptoms, and sensitivity to rejection
(572, 1068, 1069). Monoamine oxidase inhibitors have
also been shown to be effective treatments for some patients who have not responded to other antidepressant
medications (1064, 1067, 1070, 1071).
In more recent controlled trials, 6 mg/24 hours of
transdermal selegiline was compared with placebo in 177
adults with major depressive disorder in a 6-week trial
(1072). The transdermal patch was found to be more effective than placebo and was well tolerated without the
need for dietary restrictions. These findings were replicated in two subsequent studies by Amsterdam (124)
(N=365; dose, 6 mg/24 hours; duration, 6 weeks) and
Feiger et al. (125) (N=265; dose, 6–12 mg/24 hours; duration, 8 weeks).
Tranylcypromine in doses of 30–60 mg/day has been
compared with the combination of venlafaxine IR (up to
300 mg/day) and mirtazapine (up to 60 mg/day) in 109 patients with treatment-resistant depression in a 12-week
randomized trial (121). Neither the MAOI (7% remission
rate) nor the combination strategy (14% remission rate)
were particularly effective in this group of difficult-totreat depressed patients, although efficacy was compromised by the use of low tranylcypromine doses. Monoamine oxidase inhibitor therapy was significantly less well
tolerated and had a significantly higher dropout rate.
Limited evidence suggests that the nonselective MAOIs
have comparable efficacy. Tranylcypromine and phenelzine
were found to have similar response rates (44% and 47%,
respectively) in a 5-week trial of 77 patients with severe major depressive disorder who had been nonresponsive to a
TCA or SSRI medication (1073). Clinical experience suggests that some patients who fail to benefit from one of
these MAOIs may benefit from a different one—after allowing a several-week period of washout.
2. Electroconvulsive therapy
The efficacy of ECT has been demonstrated in multiple
clinical trials, including trials of real versus sham ECT. In
a meta-analysis of the efficacy of ECT in the treatment of
depressive disorders, the six trials (256 patients) that included sham ECT controls yielded a standard effect size
of 0.91 favoring real ECT, consistent with a strong effect
of active ECT (235). In the one sham ECT study that
used unilateral ECT, no difference was found, but the
treatment was not delivered sufficiently above the seizure
threshold to be effective (236). In comparison with pharmacotherapy, meta-analyses similarly show an advantage
for ECT with a standard effect size of 0.80 across 18 trials
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88
(1,144 participants) (235). Comparisons of ECT against
specific antidepressant classes show ECT to be superior
to SSRIs, TCAs, and MAOIs (236, 425). In terms of technical aspects of ECT administration, meta-analyses show
a more substantial effect of bilateral ECT than unilateral
ECT (236), with a standard effect size of 0.32 for 22 trials
and 1,408 participants (235). However, many of the included studies did not adjust the stimulus doses of ECT to
account for differences in seizure threshold across patients, which may have increased the apparent benefit of
bilateral ECT. When stimulus dosing was assessed, higher
stimulus doses relative to the patient’s seizure threshold
were associated with greater benefit than stimulus doses
closer to the seizure threshold (standard effect size = 0.73
for seven trials and 342 participants) (235). The efficacy of
ECT given twice weekly did not differ from that of ECT
given 3 times/week (236).
Much information about ECT response and specific
factors that predict response has come from the Consortium for Research in ECT (CORE) study, a large trial
funded by the National Institute of Mental Health (NIMH)
in which continuation pharmacotherapy was compared
with continuation ECT. In the acute phase of that trial in
which 253 patients were treated with bitemporal ECT
3 times/week, 79% of the sample had an acute sustained response, with remission occurring in 75% of patients after
ECT (mean number of treatments = 8 ± 3). Response to
ECT occurred rapidly, with over one-half of patients showing response by the end of the first week of treatment (240).
Suicidal ideation also resolved rapidly during the course of
ECT, with substantial resolution in 38% by the end of the
first week, 61% by the end of the second week, and 80% by
the end of the treatment course (243). Individuals who were
older (715) or who exhibited psychosis (241) or atypical features (578) had a greater likelihood of achieving remission,
although the presence of melancholic features was not associated with a greater likelihood of response (499). Also,
unlike prior studies that had shown reduced rates of remission with ECT in patients with treatment-resistant depression (1074, 1075), the CORE study found that neither
resistance to antidepressants as a whole nor resistance to
any specific class of antidepressants was associated with an
altered response to ECT (426).
In contrast to the high rates of ECT response found in
the CORE study and in meta-analyses of clinical efficacy
trials, ECT appears to have a lower rate of response when
delivered in community settings. Prudic et al. (237) examined clinical outcomes following ECT and over 6 months
of follow-up in 347 patients who received ECT at one of
seven hospitals in the New York metropolitan area. Remission occurred in only about one-third to one-half of
the sample, and two-thirds of those with remission expe-
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rienced a relapse during the follow-up period. Having residual symptoms, psychotic features, or a co-occurring
personality disorder conferred a heightened risk of relapse.
Other studies have delineated technical factors relating
to the efficacy of ECT, including stimulus intensities and
electrode placements. Sackeim et al. (253) randomly assigned 96 depressed patients to treatment with a bitemporal or right unilateral electrode placement at a low dose or
high dose relative to the patient’s seizure threshold. Patients treated with bilateral ECT had comparable response
rates regardless of stimulus dose (65% for low dose versus
63% for high dose), whereas patients receiving low-dose
right unilateral ECT had only a 17% response, and those
receiving high-dose right unilateral ECT had an intermediate response (43%). In a subsequent randomized doubleblind study of 80 depressed patients, an even higher dose
of right unilateral ECT was used (500% above the seizure
threshold). At this stimulus dose, right unilateral ECT
showed comparable efficacy to bilateral ECT (65%) and
superior efficacy to right unilateral ECT given at 50% or
150% above seizure threshold, for which the response
rates were 35% and 30%, respectively. That high-dose
right unilateral ECT has comparable benefits to bilateral
ECT has also been shown in two randomized studies by
McCall et al., one of which included 77 patients and used
right unilateral ECT at eight times the seizure threshold
(1076) and one of which included 72 patients and used a
high fixed dose of 403 millicoulombs for right unilateral
ECT (1077).
Several smaller studies have examined bifrontal electrode placement in comparison with bitemporal or right
unilateral electrode placements. Bailine et al. (1078), who
studied 48 patients with scores of 17 or higher on the 17item version of the Hamilton Rating Scale for Depression
(HAM-D-17) who were randomly assigned equally to
receive bifrontal or bitemporal ECT (mean number of
treatments = 6 ± 2.5), reported no difference in remission
rates between the two groups. Ranjkesh et al. (1079)
found no difference in HAM-D scores among patients receiving at least eight sessions of bifrontal (moderate dose,
N=15), bitemporal (low dose, N=15), or right unilateral
(high dose, N=15) electrode placement in an Iranian inpatient sample of patients with an initial score of 16 or
higher on the 24-item Hamilton Rating Scale for Depression (HAM-D-24). Similarly, Eschweiler et al. (1080)
compared the effects of six right unilateral ECT treatments (250% stimulus intensity of titrated threshold) and
six bifrontal ECT treatments (150% of threshold) over
a 3-week period in a randomized double-blind trial of
92 patients and found no difference in response rates between the two electrode placements.
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
In addition to efficacy and ECT technique, the cognitive effects of ECT have been a focus of considerable
study, typically as a part of studies examining various electrode placements. In terms of the time to recover reorientation after ECT, Sackeim et al. (253) found that patients
receiving bilateral ECT took substantially longer to regain their orientation than patients receiving right unilateral ECT, and the time to regain orientation increased
with the stimulus dose. In addition, the time to regain orientation immediately after ECT, as well as the patient’s
baseline cognitive status, predicted the patient’s cognitive
status after the ECT course and at 2-month follow-up assessment (251). Regardless of the stimulus dose of right
unilateral ECT that was used, bilateral ECT was associated
with more prominent effects on cognition at follow-up assessments (253, 1081). Relative to bilateral ECT (at one
and one-half times the seizure threshold), high-dose right
unilateral ECT (at eight times the seizure threshold) produced comparable effects on memory, and neither electrode
placement produced prolonged anterograde amnesia
(1076). Lisanby et al. (248) studied 55 patients with major
depression in a randomized double-blind trial of bitemporal and right unilateral ECT at low and high stimulus
doses and compared the patients’ function on a Personal and
Impersonal Memory Test with that of a parallel group of
normal control subjects. Bitemporal ECT was found to
cause more prominent impairments that were most notable for impersonal events and that were independent of
stimulus dose or clinical outcome. Studies of other electrode placements have shown either no difference (1080)
or beneficial effects (1078, 1079) of bifrontal electrode
placement relative to bitemporal electrode placement. Another factor that may relate to memory dysfunction is the
number of ECT treatments administered per week, with
two studies showing less prominent amnesia with twiceweekly ECT rather than ECT given 3 times/week (1082).
The cognitive effects observed in naturalistic community settings also appear to differ from those observed in
research trials (252). The seven hospitals in the community
study showed considerable variation from one another
immediately after ECT and at the 6-month follow-up assessment. These differences seemed primarily related to
differences in ECT technique across sites, with use of sine
wave stimulation and bilateral ECT being associated with
greater and more persistent cognitive effects on several
cognitive measures, compared with brief pulse and right
unilateral ECT. Given the lower efficacy rates for ECT
that were also seen in the community sample, residual or
recurrent depressive symptoms may also have contributed
to the poorer cognitive outcomes. These findings suggest
a need to optimize efficacy as well as minimize cognitive
effects in clinical practice.
89
3. Transcranial magnetic stimulation
A substantial number of studies of TMS have been conducted, but most have had small sample sizes, and the studies overall have yielded heterogeneous results. Further
complicating the interpretation of the TMS literature is
the variability in stimulation intensities (relative to the motor threshold), stimulus parameters (e.g., pulses/second,
pulses/session), anatomical localization of stimulation, and
number of TMS sessions in the treatment course. A recent
meta-analysis of 24 studies (with a total of 1,092 subjects)
found that individuals with treatment-resistant depression
were more likely to respond to TMS than to sham treatment (25% with TMS versus 17% with sham; NNT=6)
(270). However, for active treatment and for sham treatment, remission occurred in fewer than 10% of subjects
(270). Another meta-analysis that included 33 studies also
found active TMS to be more effective than sham treatment in patients with major depression but also noted substantial variability across studies (271). Studies with
stimulation intensities below 90% of motor threshold appeared to show less benefit (271). Based on a meta-analysis
that included six independent trials of left dorsolateral prefrontal cortex TMS in a total of 195 patients, older individuals and those with treatment-resistant depressive episodes
may also be less likely to respond (1083). Another metaanalysis of these six clinical trials found TMS to be no different from sham treatment overall in the treatment of major depression; however, the power within these studies to
detect a difference was generally low (273). Schutter (272)
also examined studies of TMS over the left dorsolateral prefrontal cortex and found an overall weighted mean effect size
of 0.39 for TMS based on findings from 30 studies and
1,164 patients. This meta-analysis did not find any differences in the response of individuals with medication-resistant major depression as compared with those without
documented medication resistance, nor did it find any evidence of study heterogeneity or publication bias. Multiple
earlier meta-analyses also demonstrated benefits of TMS
(1084–1087), but include an overlapping set of studies with
those assessed in more recent meta-analyses. If anything,
however, earlier studies demonstrated less efficacy for
TMS than more recent studies (272, 1088). The duration
of TMS effects has not been well studied, but one metaanalysis of 14 studies showed a robust response to TMS
compared with sham TMS after 2 weeks of treatment (standardized mean difference = −0.35; 95% confidence interval
= −0.66 to −0.04), but no statistically significant benefit of
active TMS at 2-week follow-up (1089).
The largest published trial of TMS was a randomized,
double-blind, multisite study of patients who had not responded to one to four prior trials of antidepressant therapy and were free of other medications at the time of the
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90
study (268). Subjects received sham TMS (N=146) or active TMS delivered to the left dorsolateral prefrontal cortex, 5 times/week for 4–6 weeks with 10 pulses/second and
3,000 pulses/session at 120% of motor threshold. At
weeks 4 and 6 of the study there was a trend for greater
improvement in MADRS scores in the active TMS group,
but this result did not reach statistical significance. Rates
of remission also did not differ between the two groups,
although secondary outcome measures, including the
HAM-D and response rates, did indicate a beneficial effect of TMS. In an open-label extension study of this trial
(1090), 85 subjects who had received sham TMS showed
significant reductions in MADRS scores after changing to
active TMS; 42.4% of these patients met response criteria, and 20% had remission of their depressive symptoms
by 6 weeks. Of subjects who had received active TMS and
continued to receive an additional 6 weeks of treatment
(N=73), 26% showed a response to TMS, and 11% achieved
symptom remission. Subsequent analysis of the data from
these trials (274) showed that lesser degrees of treatment
resistance were associated with better response to TMS.
The lack of a co-occurring anxiety disorder also appeared
to be associated with a better response to TMS in the
open-label extension phase of the trial.
In another large multisite trial conducted in Europe, 127
subjects with treatment-resistant depression who were being
treated with antidepressant medication (venlafaxine or mirtazapine) were randomly assigned to receive active (N=62)
or sham (N=65) TMS delivered to the left dorsolateral
prefrontal cortex, 5 times/week with 10 pulses/second and
2,000 pulses/session at 110% of motor threshold for 3 weeks.
The two groups did not differ in their degree of improvement on the MADRS, HAM-D, or BDI scales, and a similar proportion of individuals in each group (31%) were
classified as having responded to treatment (269).
Other smaller studies have compared TMS with ECT,
with variable results. One of these studies showed ECT to
be substantially more effective than TMS acutely in terms
of HRSD scores and the proportion of responders at the
end of the study, and, on the majority of outcome measures, ECT retained this benefit over TMS after 6 months
of follow-up (275). In the other studies that compared
TMS with ECT, rates of remission and response were
comparable for the two treatments, although the response
and remission rates for ECT in these studies were somewhat lower than typically reported in clinical ECT trials,
and rates of response to TMS were higher than those reported in sham controlled trials of TMS (276–278, 1091).
An additional randomized single-blind trial compared the
responses of individuals who received 2 weeks of thriceweekly unilateral ECT with the responses of individuals
who received one unilateral ECT session and four TMS
APA PRACTICE GUIDELINES
sessions each week (1092) and found no statistically significant differences in efficacy or side effects between the
two approaches. The cognitive effects of TMS and ECT
have been assessed in one open study (279), in which subjects treated with TMS reported memory to be unchanged
or improved approximately 9 days after the treatment
course as compared with unilateral ECT, which was associated with a greater degree of subjective, retrograde, and
anterograde memory difficulties shortly after the end of
the treatment course. A subsequent randomized singleblind trial (276) showed no significant difference between
individuals who received TMS and those who received
unilateral ECT when neuropsychological performance was
tested at 2 and at 4 weeks of treatment. However, there
was a trend for worsened performance in those receiving
ECT versus a trend for improved performance in those
receiving TMS.
Analysis of aggregate safety data from more than 10,000
treatment sessions with 325 patients treated at 23 clinical
sites in the United States, Australia, and Canada showed
that TMS was well tolerated, with less than 5% of subjects
leaving the study due to adverse effects and no seizures or
deaths observed (280). The most common adverse effects
were transient headaches or scalp discomfort. Overall, side
effects of treatment were mild to moderate in intensity and
dissipated over the initial week of treatment.
4. Vagus nerve stimulation
The FDA approved VNS for treatment-resistant depression based on efficacy data from two different samples, for
which acute and longer term data are available. The first
sample consisted of 60 outpatients with chronic or recurrent major depressive disorder, bipolar I disorder, or bipolar II disorder who had not responded to at least two
medication trials from different antidepressant classes. This
cohort was first followed in an open-label fashion with 10
weeks of active stimulation after a 2-week period to permit
recovery from surgery (281). On the primary outcome measure, the 28-item Hamilton Rating Scale for Depression
(HAM-D-28), 30.5% of the sample showed a response (defined as at least a 50% reduction from the baseline HAMD-28 score) and 15.3% of the sample had a full remission
of symptoms (defined as HAM-D-28 of less than 11). Response was less likely to occur in patients who had received
a greater number of unsuccessful antidepressant trials or
who had received ECT prior to VNS. This cohort was then
followed for up to 2 years naturalistically, with changes to
psychotropic medications and VNS stimulus parameters
permitted (479). In a last-observation-carried-forward analysis, response rates were 44% and 42% after 1 and 2 years,
respectively, with remission rates of 27% and 22% at 1 and
2 years, respectively (479).
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
A subsequent VNS trial was a multisite randomized
trial with 235 participants that included an acute shamcontrolled phase (282) and a longer term naturalistic follow-up phase (477) and comparison with a relatively similar
treatment-as-usual sample. In the acute phase, nonpsychotic outpatients with treatment-resistant major depressive disorder (N=210) or patients with depressed phase
bipolar disorder (N=25) received 10 weeks of active or
sham treatment after 2 weeks of recovery from implantation surgery. In terms of response (i.e., at least 50% reduction in HAM-D-24 score), there was no significant
difference with VNS treatment (15.2% response vs. 10%
for sham). These findings may be confounded by the frequent occurrence of hoarseness or voice alteration with
stimulation (281), which may have affected the blinding of
the study subjects or investigators. During the longer
term naturalistic follow-up phase, in which changes in
medication were permitted, the active VNS group received 9 additional months of VNS, and the sham group
received 12 months of VNS (282). A repeated-measures
linear regression analysis of the primary outcome measure
showed significant reductions in HAM-D-24 scores, with
response and remission rates of 27.2% and 15.8%, respectively, at the study endpoint (282). A similar but nonrandomized treatment-as-usual group (N=124) showed a
response rate of 13%, suggesting a benefit of VNS (476).
To determine whether the benefits of VNS were durable, data from the studies described earlier in this section
were combined, and the persistence of the antidepressive
response was determined (478). Of individuals who had
shown an early response (by 3 months of VNS), 66.7% and
64.6% of the overall group had maintained that response at
1 and 2 years, respectively. Of those who had shown a late
response (by 12 months of VNS), 68.5% had maintained
that response at 2 years, suggesting persistent benefits of
VNS.
An additional uncontrolled multisite European trial
showed somewhat lower rates of sustained response (44%)
at 1 year of VNS treatment, although overall response and
remission rates at 1 year were 53% and 33%, respectively
(481). Other smaller, open-label trials have been recently
reviewed and also show reductions in depressive symptoms
when VNS is used in combination with other antidepressive treatments for individuals with treatment-resistant depression (480).
Across all studies, VNS was generally viewed as tolerable (480). Rates of study dropout were low (about 1%)
during the initial 3 months of treatment (282), with about
80% of subjects continuing with VNS at the end of 2 years
(479). Voice alteration or hoarseness occurred in about
two-thirds of subjects in conjunction with stimulation
(281). Coughing occurred in about one-quarter of individ-
91
uals (281), and dyspnea and neck pain were also commonly
reported (481).
5. Complementary and alternative treatments
a. St. John’s wort
Despite a large number of trials examining St. John’s wort
(usually in the form of Hypericum perforatum extract), there
is no consensus on its efficacy in major depressive disorder.
A 2005 Cochrane meta-analysis (1093) provided a summary of treatment studies utilizing St. John’s wort for the
treatment of major depressive disorder. The published studies demonstrate heterogeneity in methods used and great
inconsistency in study outcomes. A number of doubleblind studies have demonstrated its superiority over placebo, although some have not (370, 371). In addition, St.
John’s wort may have better tolerability than TCAs and
SSRIs, and several randomized studies have shown noninferiority relative to approved antidepressant medications,
although the distinctive taste of St. John’s wort extract may
have caused some unblinding during the studies.
Among the larger and most rigorous recently published placebo-controlled trials, the studies by Shelton et
al. (371) (N=200) and Davidson et al. (370) (N=340) did not
demonstrate a difference between St. John’s wort and placebo on primary outcome measures, but Lecrubier et al.
(1094) found a significant difference between St. John’s wort
and placebo in mild to moderate depression (N=375). In
addition, a recent review of 14 short-term, double-blind
trials conducted in outpatients with mild to moderate
symptoms of major depressive disorder demonstrated that
St. John’s wort in doses of 300 mg/day and 1,800 mg/day
had efficacy superior to placebo and was generally comparable to low-dose TCA treatment (e.g., 30–150 mg/day
of amitriptyline) (105). Side effects were observed in a
lower proportion of individuals taking St. John’s wort
than among those taking a TCA (25% vs. 40%) (105).
b. S-adenosyl methionine
A number of studies have found SAMe to be efficacious in
oral doses that range from 800 mg/day to 1,600 mg/day. In
a double-blind trial, 15 inpatients with major depressive
disorder received oral SAMe or placebo for 21 days (1095).
Six of nine patients receiving SAMe demonstrated response
as defined by a reduction of 50% or more in HAM-D
scores, and depression ratings compared with placebo were
significantly lower in the SAMe group than in the placebo
group at days 14 and 21. Side effects were mild and transient. In a meta-analysis of studies comparing effects of
SAMe with those of TCAs, SAMe was found to have better
tolerability and greater efficacy in the treatment of depression, although the doses of TCAs were subtherapeutic in
some studies (381). Data from two multicenter studies also
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92
demonstrated that parenteral and oral formulations of
SAMe were comparable in efficacy to the TCA imipramine
(1096), although side effects were significantly more frequent in the imipramine-treated group. In one of the larger
controlled trials, which included 293 participants, Pancheri
et al. (382) found SAMe (administered intramuscularly at a
dose of 400 mg/day) and imipramine (administered by
mouth at a dose of 150 mg/day) to be similarly efficacious in
a 4-week trial. Other studies have focused on specific subgroups of patients, such as HIV-positive patients and postmenopausal women (1097, 1098).
c. Omega-3 fatty acids
Two large meta-analyses found benefits of omega-3 fatty
acids overall in mood disorder trials (384, 385) but also
highlighted the heterogeneity of study designs and results. The one monotherapy study of DHA for major depressive disorder in adults did not demonstrate benefit of
DHA over placebo (1099), although small trials in major
depressive disorder in children and in pregnant women
did demonstrate a benefit of monotherapy with omega-3
fatty acids (EPA and DHA) (1100, 1101).
d. Folate
In a study by Coppen and Bailey (389) that included
127 subjects, 94% of women who received fluoxetine and
500 mcg/day of folate responded to treatment, compared
with 61% of those who received fluoxetine and placebo
(p<0.005). Patients who received folate were also less
likely to report side effects (p<0.05).
e. Light therapy
In a meta-analysis, Golden et al. (395) found clinically significant benefit of bright light therapy in seasonal major depressive disorder (eight studies), with a large effect size
(0.84), and in nonseasonal major depressive disorder in
three studies with a medium effect size (0.53). However, the
authors, who were participants of an APA work group on
the topic of light therapy, determined that many of the
studies of light therapy for mood disorders had methodological flaws, including small sample sizes, with only 13% of
the studies they assessed meeting the inclusion criteria for
their meta-analysis. Bright light therapy in nonseasonal
major depressive disorder was not found to be significantly
more efficacious than placebo in trials when used adjunctively in addition to antidepressants. As determined by the
APA work group, an adequate placebo condition requires a
maximum dose of 300 lux (versus at least 3,000 lux-hours
for an active treatment condition for bright light treatment). Randomized, placebo-controlled studies have
ranged from 7–42 days in treatment duration, with provision of between 2,500–10,000 lux illuminance of white
light, with delivery time between 0.5–6 hours/day. Some
APA PRACTICE GUIDELINES
published studies were found to have bright light exposure
at levels too high to constitute a scientifically valid control
condition, and the difficulty in creating a reasonable control condition for bright light therapy may have contributed
to the limited evidence base to date. Control groups have included lower doses of white light, red light, active light
avoidance, negative air ionizer, and no treatment. Despite
heterogeneity of designs and results, evidence supports the
efficacy of bright light as a monotherapy for acute major
depressive disorder. Individualization of a regimen may be
required in terms of lux, length of exposure, and time of day
of delivery. In addition, patients should be monitored for
emergence of mania during treatment (1102).
f. Acupuncture
Assessment of the evidence base for acupuncture is complicated by the fact that many reports are in Asian languages
and therefore often overlooked by English language literature searches. Results from studies in acupuncture are difficult to interpret, because the description of the methods is
often limited and there is variability in diagnosis and in interventions (403). Wang et al. (407) published a recent
meta-analysis of eight trials of acupuncture and depression
chosen from more than 200 studies on the basis of having
a randomized design, specific diagnostic criteria for depression, and specific acupuncture interventions (manual,
electro-acupuncture, or laser). The depression criteria included DSM, International Classification of Diseases, and
Chinese Classification of Mental Disorders criteria. The
meta-analysis did not demonstrate a benefit of acupuncture
over control conditions on either response rates or remission but was based on a small number of trials with variable
methodological quality. Consequently, additional systematic study is required to assess the role of acupuncture for
major depressive disorder.
There have been few randomized, double-blind, placebocontrolled studies to inform the use of acupuncture for depression. In one published study, Allen et al. (405) compared
38 women, ages 18–45 years, who were assigned to three different groups: an acupuncture regimen specifically chosen to
address their depression, sham acupuncture, or a waiting-list
control condition. The active acupuncture group experienced a significantly greater remission rate. However, Allen
et al. (406) failed to replicate these results in a larger randomized trial, in which 151 patients with major depressive disorder received acupuncture specific for depression, sham
acupuncture, or a waiting-list condition. After 8 weeks, there
was no evidence of benefit for the acupuncture intervention
specific for depression, compared with sham acupuncture or
the waiting-list condition. Response rates were 22% for the
depression-specific acupuncture treatment and 39% for the
sham acupuncture treatment.
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
In another randomized study, Luo et al. (404) compared
effects of electro-acupuncture combined with placebo medication to the effects of amitriptyline in 241 inpatients.
Electro-acupuncture appeared equivalent to amitriptyline
at a dose of 150–175 mg/day in treating depression, with
greater improvement for symptoms of anxiety, cognitive
problems, and somatization; it also resulted in a lower side
effect burden than amitriptyline. However, no group received the placebo medication alone, and no sham treatment was used to elucidate nonspecific benefits of acupuncture treatment.
B. SPECIFIC PSYCHOTHERAPIES
1. Cognitive and behavioral therapies
a. Cognitive-behavioral therapy
In the three decades since its first evaluation as a treatment for major depressive disorder, CBT has been extensively studied in controlled trials. When meta-analyses
have quantified the efficacy of CBT compared with no
treatment or minimal treatment, effect sizes have been
fairly robust, generally near or above one standard deviation in the outcome measures (514, 1103–1106). Relative
to other treatments, estimates of CBT efficacy from
meta-analyses have been less consistent, although effect
sizes for CBT have generally been comparable to those
for other short-term forms of psychotherapy (e.g., IPT
and brief dynamic psychotherapy) (1107).
Factors relating to the administration of CBT may influence response. Some data suggest that the efficacy of
CBT may vary depending upon the severity of major depressive disorder, with less efficacy in individuals with
more severe symptoms (1108). Individuals with moderate
to severe depression may need more skilled CBT therapists to achieve therapeutic benefits (67). Other trials have
failed to show a differential response to treatments on the
basis of initial symptom severity, possibly because of lack
of statistical power (1109, 1110).
Recent research has raised questions about the relative
strengths of the cognitive and the behavioral components
of CBT. Dimidjian et al. (310) randomly assigned 241 patients with major depressive disorder to receive CBT,
behavioral activation, paroxetine, or placebo. Among patients with more severe depression, behavioral activation
had similar efficacy to medication, and both were superior
to CBT. This study shows that behavioral interventions
may be preferable to cognitive techniques for patients
with more severe depressive symptoms.
According to a data synthesis of studies conducted between 1980 and October 2004, conducted by Hollon et al.
93
(363), CBT and IPT can be as effective as medications in
the acute treatment of depressed outpatients. Comparable
rates of medication and CBT response have also been found
in a number of randomized trials. For example, Jarrett et al.
(576) compared CBT to phenelzine and placebo in a 10week randomized trial that included 108 patients with major depressive disorder with atypical features. Cognitive-behavioral therapy had comparable efficacy at achieving
response (indicated by a HAM-D score of 9 or lower), and
both were superior to placebo in an intent-to-treat analysis.
In another study, DeRubeis et al. (67) reported that among
240 patients randomly assigned to receive paroxetine, CBT,
or placebo, CBT was comparable to paroxetine but was not
clearly superior to placebo at 8 weeks. In addition, at 16
weeks, CBT and paroxetine showed comparable rates of response and remission in individuals with moderate to severe
major depressive disorder.
In subanalyses of the NIMH Treatment of Depression
Collaborative Research Program study, CBT was less effective than imipramine plus clinical management among
individuals with moderate depression (defined by scores
of 20 or higher on the HAM-D or scores of 50 or lower on
the Global Assessment of Functioning); there was also a
trend for CBT to be less effective than IPT (1108). No
differences were observed between CBT, IPT, imipramine plus clinical management, or placebo plus clinical
management among less severely depressed subjects. At
study endpoint as well as at 18-month follow-up, there
were no significant differences among these treatment
groups in degree of symptom reduction or ratings of current clinical condition. However, at the 18-month followup assessment, patients receiving IPT or CBT reported a
significantly greater capacity to establish and maintain interpersonal relationships and to recognize and understand
sources of their depression than patients in the imipramine plus clinical management group or the placebo
group (1111).
Unlike medications, CBT decreases the risk of relapse
even after this treatment is terminated (363), and continuing CBT in the maintenance phase further decreases this
risk. In a maintenance treatment study by Paykel et al. (368),
158 patients with partial remission from a major depressive episode while taking medication were randomly assigned to clinical management or clinical management and
CBT. Cognitive-behavioral therapy was given in 16 sessions over 20 weeks, with two booster sessions at 72 weeks.
Relapse reduced from 47% to 29% with CBT, and CBT was
associated with higher remission rates. Bockting et al. (497)
also compared treatment as usual (including medication)
to treatment as usual and CBT in a German outpatient
sample of 187 patients. Cognitive-behavioral therapy had
“significant protective effect” that increased with number
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94
of prior episodes. For patients with five or more prior depressive episodes, CBT lowered relapse from 72% to
46%. This study suggests that psychotherapy may have a
protective effect, especially for more severely ill patients.
b. Behavior therapy
Although numerous trials have examined the efficacy of
behavior therapy, relatively few have employed random
assignment and adequate control conditions. Two metaanalyses found behavior therapy superior to a waitinglist control condition (observed in seven of eight trials)
(487, 1107). Results of individual clinical trials have suggested that behavior therapy may be superior in efficacy
to brief dynamic psychotherapy (1112, 1113) and generally comparable in efficacy to cognitive therapy (1114–
1117) or pharmacotherapy (283). One post hoc examination of clinical trial data found that response to behavior
therapy may be more likely in patients with less initial severity of major depressive disorder symptoms (1118),
but other studies have not found this relationship (1119–
1121).
More recently, “dismantling studies” comparing the full
CBT package to some of its elements suggest that behavioral activation, the behavioral component of CBT, may
be as efficacious or more efficacious than CBT as a whole,
particularly for patients with greater depressive severity
(310, 1122). Behavioral activation not only outperformed
CBT and placebo with respect to more severely depressed
patients, but it was as efficacious as medications regardless
of severity (310) and more enduring following treatment
termination (288). In addition, activity scheduling, a behavioral activation treatment in which patients learn how
to increase the number of pleasant activities and interactions with their environment, was found in a meta-analysis to be an effective treatment for depression (706).
2. Interpersonal therapy
Like CBT, IPT was developed to treat patients with major
depressive disorder and has demonstrated efficacy in a
series of randomized clinical trials (1123, 1124). In the
NIMH Treatment of Depression Collaborative Research
Program study, IPT had greater efficacy than pill placebo
plus clinical management and was comparable to imipramine plus clinical management for patients with more
severe major depressive disorder, whereas cognitive therapy was not superior to placebo. Among patients with
mild depressive severity (defined as scores less than 20 on
the HAM-D or greater than 50 on the Global Assessment
of Functioning scale), IPT, CBT, and imipramine plus
clinical management did not differ from placebo plus clinical management (1108). The degree to which patient and
therapist can resolve the interpersonal crisis on which IPT
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focuses (e.g., a role transition) appears to correlate with
symptomatic improvement (1125).
Other studies have found IPT effective in treating
pregnant and postpartum women with major depressive
disorder (743, 1126) and depressed patients in a developing country (351). A controlled trial of IPT has also demonstrated its effectiveness for depressed primary care
patients (1127). After 8 months, the proportions of patients treated with IPT, nortriptyline, or usual care who
achieved remission were 46%, 48%, and 18%, respectively.
In a study of depressed HIV-positive patients, greater improvements were observed after IPT or IPT plus imipramine than after supportive psychotherapy or CBT (316).
However, a large recent study found no benefit for IPT
over clinical management in depressed cardiac patients
(807).
Many trials have been conducted comparing IPT, both
as monotherapy and augmentation, to various control
conditions and active comparators, both in acute phase
treatment and continuation and maintenance therapy.
Generally, IPT is superior to treatment as usual and is an
effective augmentation strategy for patients receiving
pharmacotherapy. A meta-analysis of 13 studies of IPT
conducted from 1974 to 2002 reported that, in nine of the
studies, IPT was superior to placebo (1123). In addition,
IPT was more efficacious than CBT. However, the combination of IPT and medications was not significantly
more effective than medication monotherapy for acute or
prophylactic treatment.
3. Psychodynamic psychotherapy
Psychodynamic psychotherapy has been used widely in
clinical practice for the treatment of patients with depressive symptoms and syndromes and is sometimes preferred
by patients (361). However, its efficacy in major depressive disorder has not been adequately studied in controlled trials. Using the available evidence to determine
the efficacy of psychodynamic psychotherapy in the treatment of major depressive disorder is complicated by several
problems. In some early studies, variants of psychodynamic psychotherapy served as a nonspecific comparison
treatment to other psychotherapeutic interventions, but
the details of the psychodynamic psychotherapy employed
were poorly defined (1107). Subsequently, some clinical
trials of psychodynamic psychotherapy have reported
short- and long-term therapeutic benefits (as described in
references 1128–1130), but few of these trials were randomized or assessed treatment fidelity; some included
concomitant pharmacotherapy, and most studied patients
with a multiplicity of symptoms and diagnoses, such as depressed patients who did not meet the DSM-IV criteria
for major depressive disorder. These limitations make it
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
difficult to draw conclusions from meta-analyses that incorporate a variety of study populations and designs (286,
1130, 1131). A recent meta-analysis (1132) acknowledged
that the quality of available studies on psychodynamic
psychotherapy for treatment of depression was not optimal. In addition, use of low-quality studies in meta-analyses of psychotherapy may lead to overestimations of
effect sizes (1133). With these caveats, some findings from
meta-analyses of short-term (1132) and long-term (1130)
psychodynamic psychotherapy suggest possible benefits
in individuals with depressive symptoms (1132) and suggest that long-term psychodynamic psychotherapy may
have beneficial effects in individuals with depressive and
anxiety symptoms (1130). To confirm these results and extend them to individuals diagnosed with major depressive
disorder, further research with more rigorous study designs will be needed.
4. Marital therapy and family therapy
Reviews have concluded that marital therapy is effective
for treating depressive symptoms and reducing risk for relapse (1134, 1135). In a recent meta-analysis of eight marital therapy trials, marital therapy had comparable efficacy
to individual psychotherapy for the treatment of depression (1136). A lower dropout rate was found for marital
therapy than for medication therapy, although this result
was heavily influenced by a single study. Marital therapy
was superior in treating depressive symptoms, compared
with minimal or no treatment. These findings were weakened by methodological problems affecting most studies,
such as the small number of cases available for analysis in
almost all comparisons, and the significant heterogeneity
among studies.
Results from individual studies suggest that the efficacy
of marital therapy may depend on whether marital distress
is present. In one study, a greater proportion of depressed
subjects with marital distress responded to marital therapy
than to cognitive therapy (88% vs. 71%), but among depressed subjects without marital distress, a greater proportion responded to cognitive therapy than to marital therapy
(85% vs. 55%) (1137). In another study of depressed subjects with marital discord, marital therapy and CBT were
equally effective and both were more effective than a waiting-list condition (1138). A pilot randomized trial found
“conjoint” (marital) IPT for depressed married women
equipotent to individual IPT in alleviating depression and
superior in improving marital satisfaction (1139).
A randomized controlled trial of antidepressant drug
therapy in comparison to couple therapy for depressed outpatients found a lower dropout rate and greater improvement in subjective symptoms of depression, at no greater
cost, for the couple therapy group (342). Patients recruited
95
during a psychiatric hospitalization for major depressive
disorder were randomly assigned to pharmacotherapy
alone; combined pharmacotherapy and cognitive therapy;
combined pharmacotherapy and family therapy; and combined pharmacotherapy, cognitive therapy, and family therapy. Patients who received treatment that included a family
therapy component were more likely to improve and had
significant reductions in interviewer-rated depression and
suicidal ideation, compared with those whose treatment did
not include family therapy (343).
5. Problem-solving therapy
Some studies have reported modest improvement in subjects with mild depressive symptoms treated with problem-solving therapy. For example, Dowrick et al. (1140)
treated 452 subjects with depressive or adjustment disorders, comparing groups that received eight sessions of
problem-solving therapy to control groups given six sessions of group preventive education. At 6 months, the authors found a 2.6-point difference on the BDI favoring
problem-solving therapy (NNT=6). Treatment effects at
1 year did not differ. Problem-solving therapy may have
advantages over usual care for home-bound geriatric patients with depressive symptoms (1141). Unfortunately,
usual care often means little care.
Alexopoulos et al. (335) reported that 12 sessions of
problem-solving therapy were superior to supportive
psychotherapy for depressed geriatric patients with major
depressive disorder and executive dysfunction. Another
study showed problem-solving therapy to have greater
benefit than usual care in preventing depression (1142).
6. Group therapy
A mostly European body of research suggests that the individual psychotherapies validated in treating depression
also work in group format. Most of these studies have
sought to demonstrate efficacy rather than exploring the
technical aspects of group therapy.
Group cognitive therapy has shown benefits in the acute
treatment of major depressive disorder. For example, Ayen
and Hautzinger (347) randomly assigned 51 depressed,
menopausal women for 3 months of weekly, 2-hour sessions of cognitive group therapy, of group supportive psychotherapy, or a waiting list. Both active treatments were
well tolerated and relieved depressive and menopausal
symptoms better than the control condition. At 1-year follow-up, group CBT was more beneficial than group supportive therapy. In contrast, group CBT was ineffective in
treating dysthymic disorder. Ravindran et al. (293) found
sertraline superior to placebo but 12 weeks of group CBT
no better than placebo and ineffective in augmenting sertraline in treatment of patients with dysthymia.
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96
McDermut et al. (1143) conducted a meta-analysis of
48 research reports assessing the efficacy of group therapy
for the treatment of depression in individuals with various
types of depressive disorders (depressive spectrum disorders). Analyses suggested that participants in treatment
showed significant clinical improvement.
Forms of group CBT have also shown promise in lowering relapse risk. Bockting et al. (497) reported that for the
41% of 187 patients with remission who had a history of at
least five episodes of recurrent major depressive disorder,
augmenting usual treatment with brief group CBT lowered relapse rates from 72% to 46% over a 2-year period.
Teasdale et al. (498) found that group mindfulnessbased cognitive therapy as an augmentation strategy was
beneficial relative to treatment as usual in reducing relapse rates over 60 weeks for 145 patients with recurrent
depression who reported at least three prior major depressive episodes.
Interpersonal psychotherapy has also been adapted to a
group format (1144). Although IPT is less well studied
than CBT, small trials of group IPT suggest its benefits as
both a preventive intervention (350) and a treatment for
postpartum depression (349). A group combining interpersonal and cognitive elements improved outcome relative to fluoxetine alone among patients with dysthymia
who responded to fluoxetine (1145).
C. PSYCHOTHERAPY COMBINED
WITH PHARMACOTHERAPY
Although many psychiatrists prefer to use a combination of
psychotherapy and pharmacotherapy to treat patients with
depression, controlled studies conducted in the 1970s and
1980s did not consistently find a significant advantage for
routinely combining therapies, compared with one or the
other treatments provided alone (1146). Part of the problem in establishing the additive value of psychotherapy and
pharmacotherapy in these early studies was methodological: the specific effects of each modality (i.e., over and above
the so-called nonspecific effects of therapeutic support and
placebo-expectancy factors) are relatively modest, and
none of the early studies of combined therapy had the statistical power to reliably detect such small effects. Consistent with this appraisal, a meta-analysis of these early
studies found an average effect size of about 0.3 (1147),
which is both a clinically significant effect and an advantage
that would usually not be found to be statistically significant in a study of 100 or fewer patients. A meta-analysis of
individual patient data performed by Thase et al. (359),
which compared remission rates of nearly 600 patients
treated in studies of CBT, IPT, and IPT in combination
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with either imipramine or nortriptyline, confirmed a modest overall advantage for combined treatment versus CBT
or IPT alone but found a differential impact linked to severity and history of recurrent depressive episodes. Specifically, whereas combined treatment had a small advantage
over psychotherapy alone among patients with less severe
depression, there was a fourfold difference in remission
rates among the subset of patients with more severe, recurrent depressive episodes.
The advantage of combined treatment over pharmacotherapy alone in more severe depression was evident in a
well-controlled inpatient study of Schramm et al. (285).
Conducted in Germany, this 5-week trial included 124 hospitalized patients with major depressive disorder; results
showed a 70% response rate to IPT plus pharmacotherapy,
compared with a 51% response rate to pharmacotherapy
alone. In a Swiss study in which 74 outpatients were randomly assigned to receive 10 weeks of clomipramine plus
psychodynamic therapy or clomipramine alone, the combination treatment produced greater improvements in global
functioning, greater cost savings, lower rates of hospitalization, and fewer lost work days (1148).
Keller et al. (362) examined the outcomes of more than
600 patients with chronic depression who were randomly
assigned to treatment with the antidepressant nefazodone
or a form of CBT (cognitive behavioral analysis system of
psychotherapy [CBASP]) singly or in combination. The
authors found a large additive advantage for the two treatments in combination. Specifically, response rates for combined treatment were approximately 20% higher at the
end of 12 weeks of treatment, compared with the monotherapies, which were comparably effective. It is noteworthy
that patients receiving combined treatment experienced the
earlier benefit that characterized the pharmacotherapy as
well as the later emerging benefit that characterized the
psychotherapy (362). A post hoc analysis of these results
revealed that the advantage of the combined approach was
explained by a broader spectrum of efficacy: pharmacotherapy alone was significantly less effective than CBASP
among the subset of patients with a history of childhood
trauma, whereas the opposite trend was evident among
the patients treated with psychotherapy alone (1149). Patients with chronic depression were thus more likely to
benefit from combined treatment whether or not they had
a history of early adversity.
In the STAR*D study, patients with depression who did
not have remission following an initial 12-week course of
citalopram therapy were offered the opportunity to add
or change to Beck’s model of cognitive therapy in addition
to the various pharmacotherapy options being studied.
Among those who opted to add a therapeutic adjunct to
ongoing citalopram, about one-third consented to be ran-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
domly assigned to strata that included both cognitive therapy and medications (buspirone or bupropion). Results at
the end of 12 weeks of therapy indicated that cognitive therapy was as effective as medication augmentation, although
patients opting for combined pharmacotherapy responded
faster (369).
One historic limitation of the literature on combined
treatment of depression has been that a vast majority of
studies have concerned cognitive therapy and IPT, and
there has been a dearth of studies on the more widely practiced forms of psychodynamic psychotherapy. An informative series of studies by one group of investigators in the
Netherlands has helped to partly address this issue. The
first trial compared outcomes of 167 outpatients with depression across 6 months of treatment with either algorithm-guided antidepressant pharmacotherapy alone or
pharmacotherapy combined with a manual-based form of
time-limited dynamic psychotherapy (1150). Significant
differences favored combined treatment with respect to
retention in treatment and the likelihood of remission. A
secondary analysis determined that the advantage of combined treatment was largely explained by the large difference among patients with co-occurring Axis II disorders
(1151). In a second study of 191 depressed outpatients,
time-limited dynamic therapy alone was compared against
psychotherapy in combination with algorithm-guided
pharmacotherapy (1152). In this trial, there were significant differences favoring combined therapy on patientrated outcomes, although the numeric difference between
groups on remission rates was not statistically significant.
The investigators next conducted a pooled analysis of the
data from these two trials, also including a third smaller
study that did not include a combined therapy arm (361).
The analysis included data for more than 300 depressed
outpatients and confirmed the advantage of combined
treatment over the monotherapies across studies on most
outcome variables.
Two meta-analyses of study results have confirmed the
advantage of combining pharmacotherapy and various
forms of time-limited psychotherapies (360, 1153). The latter report confirmed that the advantage was larger among
studies of patients with more severe symptoms and among
those with more chronic depressive disorders (1153).
D. LACK OF RESPONSE TO PHARMACOTHERAPY
IN THE ACUTE PHASE
1. Maximizing initial treatments
Several studies have shown improved efficacy with higher
doses of medication, supporting the strategy of increasing
the medication dose for patients who do not respond to an
97
initial trial of a medication. As an example, Bech et al. (1154)
conducted a randomized controlled trial in which patients
meeting the criteria for major depressive disorder were
randomly assigned to receive placebo or citalopram in doses
of 10 mg/day (N=129), 20 mg/day (N=130), 40 mg/day
(N=130), or 60 mg/day (N=129). Treatment continued
for 6 weeks, and depressive symptoms were measured by
21-item Hamilton Rating Scale for Depression, MADRS,
Clinical Global Impression, and 56-item Symptom Checklist. The percentages of patients lost to follow-up were
9% for placebo, 7% for citalopram at 10 mg/day, 2% for
citalopram at 20 mg/day, 2% for citalopram at 40 mg/day,
and 3% for citalopram at 60 mg/day (nonsignificant p values). The 10- and 20-mg doses were more efficacious than
placebo, but they were inferior to the 40- and 60-mg doses
(p<0.05). The 20-, 40-, and 60-mg doses had significantly
more side effects than placebo, measured by dropout rates
due to side effects (p<0.05).
2. Changing to other treatments
The recently completed STAR*D trial examined various
strategies for patients with treatment-resistant depression.
STAR*D was a multisite, multistep, prospective randomized controlled trial comparing treatments and treatment
strategies in outpatients with major depressive disorder
(48). The study provided data on treatment effectiveness,
or “real world” outcomes in typical patients, making the
results generalizable to standard practice. The study was
organized into four levels. In level 1, 2,876 outpatients
received citalopram for up to 14 weeks. In level 2, nonresponders (N=1,493) were offered three alternatives, which
were selected based on patient choice: change to another
medication (N=727), augment citalopram with another
medication (N=565), or start psychotherapy (N=147). If
the patient changed to another medication, he or she was
randomly assigned to receive sertraline, bupropion SR, or
venlafaxine XR. Patients who chose medication augmentation were randomly assigned to augment citalopram
with bupropion SR or buspirone. Patients who agreed to
start psychotherapy were randomly assigned to change to
cognitive therapy (discontinuing citalopram) or to augment with cognitive therapy (continuing citalopram). For
patients who did not respond to level 2, level 3 offered two
alternatives: changing or augmenting with another medication. Patients in the change group were randomly assigned to receive mirtazapine (N=114) or nortriptyline
(N=121) for up to 14 weeks. Patients in the augmentation
group were randomly assigned to receive lithium (N=69)
or triiodothyronine (N=73) for up to 14 weeks. Finally,
level 4 randomly assigned nonresponders from level 3
to receive tranylcypromine (N=58) or the combination of
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98
venlafaxine XR and mirtazapine (N=51). STAR*D therefore
provides data for several randomized controlled trials of
change or augmentation of medications at various stages.
Two such studies based on STAR*D data provide evidence
for continued efficacy of medication augmentation (429)
and medication change (471) for treatment-resistant depression. Remission rates were equivalent and approximately 25% upon changing from citalopram to either an
SSRI or SNRI or bupropion at the second step; there was
no difference in remission between changing to either
mirtazapine or nortriptyline at the third step.
A number of previous studies evaluated changing from
an SSRI to another SSRI, changing from an SSRI to an
SNRI, and changing from an SSRI to bupropion or mirtazapine. These previous studies were either small in size
or, in the vast majority of instances, were neither randomized nor blinded. A few trials have been conducted in
which patients who did not respond to an initial antidepressant medication were changed to a non-MAOI antidepressant medication from the same pharmacological class
(e.g., from one TCA to another) or to one from a different
pharmacological class (e.g., from a TCA to an SSRI). Although results from these trials have been variable, up to
50% of patients have been found to respond (i.e., have symptom improvement of at least 50%) to a second non-MAOI
antidepressant medication trial—even when the second antidepressant was from the same class as the first (421). Data
regarding the types of treatment-resistant patients who are
most likely to benefit from particular changes in medication are limited.
3. Augmenting and combining treatments
Traditionally, augmentation agents with the most evidence for efficacy have included lithium and thyroid hormone for partial responders to traditional antidepressant
medications (1155). Recent studies have significantly advanced the literature now with the two augmentation randomized controlled trials in STAR*D (429, 446) and the
use of adjunctive aripiprazole (453, 1156). In the most
recent large-scale trial—a component of the STAR*D
study—lithium augmentation of citalopram was neither
particularly well tolerated nor more effective than thyroid
augmentation (446).
The second-step augmentation trial in the STAR*D
study evaluated the comparative efficacy of add-on sustained-release bupropion and add-on buspirone in patients who had not achieved adequate remission status
following an initial trial with citalopram. Both agents as
adjuncts were associated with remission rates of around
30% on primary outcome measures. Patients who did not
have remission with up to 12 weeks of citalopram therapy were as likely to benefit from adjunctive buspirone
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(15–60 mg/day) as they were to benefit from adjunctive
bupropion (150–400 mg/day) (429). However, adjunctive
treatment with bupropion SR was superior to adjunctive
buspirone on a number of key secondary measures (224).
The findings of 16 placebo-controlled, randomized
clinical trials of second-generation antipsychotic augmentation therapy for patients with major depression disorder
(N=3,480) have recently been evaluated in a meta-analysis
(448). Augmentation with a second-generation antipsychotic agent was significantly more effective than placebo
in terms of rates of response and remission. Although aripiprazole has received FDA approval as an adjunct to second-step antidepressant medications for patients who had
not achieved satisfactory response to at least two prior antidepressant medication trials, this meta-analysis showed
no differences in response or remission rates among the individual medications (448). Discontinuation rates for adverse effects were also higher in the active augmentation
groups compared with placebo, suggesting that such effects
need to be taken into consideration when choosing to augment antidepressant response with a second-generation antipsychotic agent. To date, few data from controlled studies
address the longer term efficacy or side effects of combining antidepressants and antipsychotics.
Combining an SSRI and a TCA induced a rapid antidepressant response in one preliminary study (1157). In a
second study, patients taking this combination also had a
greater likelihood of remission, compared with patients
receiving monotherapy with an SSRI or a TCA (1158).
The efficacy of combining mirtazapine and an SSRI was
demonstrated in one placebo-controlled study (432). Mirtazapine and venlafaxine led to a 13.7% remission rate in
patients who had not responded to three prior medication
trials as part of the STAR*D study (121). Case reports suggest that stimulant medications may be effective adjuncts
to antidepressant medication therapy (205), although the results of larger scale clinical trials have not demonstrated
efficacy (462, 463).
E. CONTINUATION TREATMENT
Although randomized controlled trials of antidepressant
medications in the continuation phase are limited, the
available data indicate that patients treated for a first episode of uncomplicated major depressive disorder who
exhibit a satisfactory response to an antidepressant medication should continue to receive a full therapeutic dose of
that agent for at least 16–20 weeks after achieving and maintaining full remission (105, 225, 495).
Two clinical trials have examined the effects of continuation treatment following an acute course of ECT. In a
randomized double-blind trial that included 84 individu-
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Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
als with major depressive disorder whose symptoms had
remitted with ECT, the combination of nortriptyline (target steady-state level, 75–125 ng/mL) plus lithium (target
steady-state level, 0.5–0.9 mEq/L) was associated with
lower relapse rates over the 24-week trial (39%) than either nortriptyline alone (60%) or placebo (84%) (489). A
subsequent trial found that continuation pharmacotherapy with lithium plus nortriptyline (N=94) was comparable
in efficacy to continuation ECT (N=89) in maintaining
remission (46.3% versus 46.1%) after a successful acute
course of ECT (234). The group receiving medication reported a greater number of treatment-emergent side effects than the ECT group, but there were no differences
in cognitive impairment reported between the treatment
groups.
A few studies have examined treatment with psychotherapeutic interventions administered in the continuation phase. One study found that among patients who
responded to acute treatment with cognitive therapy, those
who continued this treatment over 2 years had lower relapse rates than those who did not have continuation
treatment (493). Results from a series of studies (365, 367,
494) suggest that CBT may be an effective continuation
treatment following antidepressant medication therapy
for preventing relapse (364).
In a randomized controlled trial of cognitive group
therapy as an adjunct to treatment as usual, Bockting et al.
(497) studied 187 patients with recurrent major depressive
disorder who were currently in remission. Cognitive group
therapy was found to be effective in preventing relapse/
recurrence, and this protective effect increased in concert
with the number of previous depressive episodes.
Hollon et al. (68) assessed 104 patients with major depressive disorder who had responded to cognitive therapy,
pharmacotherapy, or placebo and had remained improved
during a 12-month continuation phase. Patients were withdrawn from treatment and followed for an additional 12
months. Cognitive therapy patients, who were allowed no
more than three booster sessions over that year, had a lower
rate of relapse (31%) than those withdrawn from medication (76%). They also exhibited no greater likelihood of
depressive relapse than patients who continued pharmacotherapy (47%), suggesting possible lasting benefits of
cognitive therapy.
F. MAINTENANCE TREATMENT
The multicenter Prevention of Recurrent Episodes of
Depression With Venlafaxine for Two Years (PREVENT)
study was designed to evaluate patients with recurrent
unipolar major depressive disorder randomly assigned to
receive venlafaxine XR or fluoxetine. At the end of a 10-
99
week acute phase treatment, response rates were 79% for
both venlafaxine XR and fluoxetine, with remission rates
being 49% and 50%, respectively. In the 6-month continuation phase, response rates were 90% (venlafaxine XR)
and 92% (fluoxetine), with rates of sustained remission of
52% and 58%, respectively. The cumulative probability of
recurrence through the first 12 months of the maintenance
phase treatment was 23.1% for venlafaxine and 42% for
placebo. The cumulative probability of recurrence through
the second 12 months of maintenance treatment was 8%
in the venlafaxine XR group and 44.8% in the placebo group
(226, 1159).
There have been fewer investigations of the effectiveness
of psychotherapy in the maintenance phase. In one study,
maintenance cognitive therapy delivered over 2 years was as
effective as maintenance medication for recurrent major
depressive disorder (514). Other reports indicate that IPT
may effectively lengthen the interepisode interval for
patients with recurrent depression who do not receive
medication (289, 314, 513, 1056). Maintenance CBT as
augmentation to medication prevented relapse relative to
medication plus treatment as usual (368, 497, 1160).
Monthly maintenance psychotherapy with CBASP was
more effective over a 1-year period than an assessmentonly control condition for patients with chronic depression who had responded to acute treatment and remained
improved in continuation therapy with CBASP (1161). A
6-year follow-up of patients treated with medication and
continuation CBT found weakening but continuing ongoing benefits lasting as long as 3.5 years after completing
CBT (1162). Research on cognitive therapy has explored
the concept of an enduring benefit by acquiring persistent
skills that reduce the risk of depressive relapse after treatment has ended (68, 1110).
The combined use of psychotherapy, such as CBT,
cognitive therapy, or IPT, and pharmacotherapy in the
maintenance phase has also been considered by investigators. Some results suggest that the combination of antidepressant medications plus psychotherapy may be
additionally effective in preventing relapse over treatment
with single modalities (314, 365, 506, 515, 516). However,
in individuals older than age 70 years who received maintenance treatment with paroxetine and clinical management, interpersonal therapy and placebo, paroxetine and
interpersonal therapy, or placebo and clinical management, the combination of paroxetine and interpersonal
therapy offered no benefits over paroxetine and clinical
management and each were superior to the other treatment conditions (729).
Electroconvulsive therapy has also been used in the
maintenance phase. Evidence for its benefits comes
largely from case reports and case series (1163–1168), al-
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10 0
though a retrospective case-control study (1169) and a
randomized prospective trial in older adults (730) demonstrated longer times to recurrence with use of maintenance
ECT. The optimal frequency, duration, and method of
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discontinuing maintenance ECT treatment have not been
systematically studied, but typically ECT is tapered gradually with a return to more frequent treatments if depressive symptoms emerge (501).
Part C
FUTURE RESEARCH NEEDS
Notable progress has been made in our understanding of
major depressive disorder and its treatment. However,
there are still many unanswered questions about optimizing and individualizing treatment. The following areas require additional study.
To “personalize” care, and someday even prevent depression, we must understand factors that cause it. In the
nearer term, science can focus on predictors of benefit and
adverse effects of specific treatments. Potential causes of
depression or moderators of treatment response may be
found through genomics, proteomics, physiological markers, personality traits, personal experiences, co-occurring
conditions, or clusters of specific depressive symptoms.
Culture, race, and ethnicity merit study in shaping treatment selection and predicting response and side effects.
Even if science were to offer perfect and personalized
treatments for depression, patients must be able to gain
access to care and adhere to recommended interventions.
Thus, research must develop better ways to deliver treatment, optimizing effectiveness as well as efficacy. Research should also consider the cost-effectiveness of care
and effects of treatment on functioning and quality of life.
As the U.S. population ages and co-occurring illnesses
become more common, studies are needed on ways to integrate care for depression with treatment for other psychiatric and medical problems. Most studies of major
depressive disorder have examined the acute phase of treatment. More research is required on the continuation and
maintenance phases. Questions abound on the persistence
of biological and psychosocial treatment effects, when
treatment may safely be discontinued, how recurrent depression differs from chronic varieties in the long term, and
more.
The science of psychotherapy research continues to
evolve. We need to understand how specific types of therapy compare to one another in the treatment of major depressive disorder and how to select a treatment for an
individual. Research must disentangle nonspecific factors
from the unique features of a theoretically derived approach. It would be important to determine the components of specific psychotherapies that are responsible for
efficacy, the patient-specific factors that moderate the efficacy of these therapies, the indications for using a particular psychotherapy, and the optimal duration and
frequency of psychotherapy for particular patient subgroups, types of psychotherapy, or phases of depression
treatment. Outcome measures of psychotherapy studies
should not only examine acute symptom response but also
whether psychotherapies have enduring, protective effects in averting relapse and recurrence of depression after
treatment has ended. A manual-based model of psychodynamic therapy for depression (1170) may be helpful in
the development of evidence concerning this approach.
Strategies for sequencing psychotherapy in the overall
treatment of major depressive disorder and for combining
psychotherapy (either with pharmacotherapy or another
psychotherapy) merit further study.
Much work remains to be done on medication intervention in depression. We should address the comparative
efficacies, relative short- and long-term side effect profiles,
and specific clinical indications of different antidepressant
medications, augmentation strategies (e.g., second-generation antipsychotic medications, lithium, thyroid hormone) and combination treatment approaches (e.g., SSRIs
and other moieties). This would include determining if
particular treatments or combinations of treatments have
differential efficacy in specific subgroups of patients with
depression (e.g., patients with psychotic depression) and,
for medications other than the TCAs, whether relationships exist between medication blood levels and therapeutic responses or side effects. Initial studies of monotherapy with second-generation antipsychotic agents appear
promising, but additional study of the acute and long-term
benefits and side effects is essential. The definition and implications of treatment-resistance for treatment selection
also requires further clarification.
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
Electroconvulsive therapy remains the treatment of best
established efficacy against which other stimulation treatments (e.g., VNS, deep brain stimulation, TMS, other
electromagnetic stimulation therapies) should be compared. Approaches to reducing cognitive side effects of
ECT, speeding response to ECT, or determining the indications and best methods for maintenance ECT could improve patient care. More research is also needed on the
optimal approaches (e.g., treatment schedule, stimulation
parameters) for delivering newer stimulation therapies. Additional research on light therapy would be helpful, including determining its effectiveness as adjunctive treatment in
nonseasonal major depressive disorder or as a primary
treatment for seasonal major depressive disorder in the
101
maintenance phase. Given patients’ frequent use of complementary therapies, additional research on these therapies, including acupuncture, is warranted. Further study of
exercise in acute and maintenance treatment of depression
would also be useful, including assessment of the benefits of
exercise in minimizing side effects of the other therapies
and in optimizing health, functioning, and quality of life.
In time, brain imaging, genomics, proteomics, and
other recent advances in neuroscience should help us
“carve nature along its joints,” allowing major depressive
disorder to be broken into discrete diseases with defined
and personalized treatments. In the meantime, clinical investigation focused on existing and novel treatment strategies remains essential.
Appendix
EDUCATIONAL RESOURCES FOR PATIENTS AND FAMILIES
Academy of Cognitive Therapy
http://www.academyofct.org
California Teratogen Information Service and Clinical Research
Tel: 1–800–532–3749 (CA only)
Tel: (610) 543–2131
http://www.otispregnancy.org
ConsumerLab.com
Tests herbal and vitamin products for purity and posts the
results on the Web
http://www.consumerlab.com
Depression After Delivery, Inc.
91 East Somerset Street
Raritan, NJ 08869
Tel: (800) 944–4773
http://www.depressionafterdelivery.com
Depression and Bipolar Support Alliance
730 Franklin Street
Suite 501
Chicago, IL 60610–7224
Tel: (312) 642–0049
Tel: (800) 826–3632
http://www.ndmda.org
Healthy Minds, Healthy Lives
American Psychiatric Association
http://www.healthyminds.org
International Foundation for Research and Education on Depression
2017-D Renard Court
Annapolis, MD 21401
Tel: (410) 268–0044
http://www.ifred.org
International Society of Interpersonal Psychotherapy
http://www.interpersonalpsychotherapy.org
KidsHealth.org
http://www.kidshealth.org
Massachusetts General Hospital Women’s Mental
Health Program
http://www.womensmentalhealth.com
Mental Health America
2000 N. Beauregard Street
6th Floor
Alexandria, VA 22311
Tel: (703) 684–7722
Tel: (800) 969–6MHA (6642)
TTY Line: (800) 433–5959
http://www.nmha.org
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
10 2
MentalHelp.net
http://www.mhnet.org
Motherisk.com
Database maintained by the Toronto Hospital for Sick
Children
http://www.motherisk.com
NARSAD
60 Cutter Mill Road
Suite 404
Great Neck, NY 11021
Tel: (516) 829–0091
http://www.narsad.org
National Alliance on Mental Illness
Colonial Place Three
2107 Wilson Blvd., Suite 300
Arlington, VA 22201
Tel: (703) 524–7600
Help Line: (800) 950-NAMI [6264]
http://www.nami.org
National Center for Complementary and
Alternative Medicine
National Institutes of Health
9000 Rockville Pike
Bethesda, MD 20892
http://nccam.nih.gov/
National Institute of Mental Health
Depression Information Program
6001 Executive Boulevard
APA PRACTICE GUIDELINES
Room 8184, MSC 9663
Bethesda, MD 20892–9663
Tel: (301) 443–4513
TTY Line: (301) 443–8431
http://www.nimh.nih.gov/health/topics/depression/
index.shtml
National Institute of Mental Health
Mental Health Topics
http://www.nimh.nih.gov/health/topics/index.shtml
National Institute of Mental Health
Public Information and Communications Branch
6001 Executive Boulevard
Room 8184, MSC 9663
Bethesda, MD 20892
Tel: (866) 615–6464
http://www.nimh.nih.gov/publicat/index.cfm
National Library of Medicine
U.S. government online repository of articles published
in peer-reviewed medical journals
http://www.ncbi.nlm.nih.gov/
entrez/query.fcgi?db=PubMed
Postpartum Support International
http://postpartum.net
Substance Abuse and Mental Health Services
Administration’s National Mental Health
Information Center
http://mentalhealth.samhsa.gov/
INDIVIDUALS AND ORGANIZATIONS THAT SUBMITTED
COMMENTS
M.T. Abou-Saleh, M.B.Ch.B., M.Phil., Ph.D.,
F.R.C.Psych.
Jonathan E. Alpert, M.D., Ph.D.
Robert J. Barth, Ph.D.
Carl C. Bell, M.D.
Franco Benazzi, M.D., Ph.D.
Joseph Berger, M.D.
Dan G. Blazer, M.D., Ph.D.
David W. Brook, M.D.
Joseph R. Calabrese, M.D.
Anita H. Clayton, M.D.
C. Edward Coffey, M.D.
Mirean Coleman, M.S.W., L.I.C.S.W., C.T.
C. Deborah Cross, M.D.
Mark A. Demitrack, M.D.
Wayne H. Denton, M.D., Ph.D.
P. Murali Doraiswamy, M.D.
Javier I. Escobar, M.D., M.S.
Giovanni Andrea Fava, M.D.
Max Fink, M.D.
Tony Fowke, A.M.
Andrew J. Francis, M.D., Ph.D.
Glen O. Gabbard, M.D.
Gary G. Gintner, Ph.D.
Leslie Hartley Gise, M.D.
Michael J. Gitlin, M.D.
Predrag Gligorovic, M.D.
Jack M. Gorman, M.D.
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
Practice Guideline for the Treatment of Patients With Major Depressive Disorder, Third Edition
Ellen Grabowitz, M.D.
Michael F. Grunebaum, M.D.
John G. Gunderson, M.D.
Ana Maria B. Gutierrez, M.D.
Steven D. Hollon, Ph.D.
Joseph J. Horak, Ph.D.
Douglas G. Jacobs, M.D.
Bradley R. Johnson, M.D.
Lewis L. Judd, M.D.
Gabor I. Keitner, M.D.
James H. Kocsis, M.D.
Lorrin M. Koran, M.D.
Milton Kramer, M.D.
Arthur Lazarus, M.D., M.B.A.
Ellen MacKenzie, M.D.
Lauren Marangell, M.D.
Kathleen Ries Merikangas, Ph.D.
Helen Millar, M.D.
Stuart A. Montgomery, M.D.
Anthony T. Ng, M.D.
Mary Olinger, M.D.
Maria Oquendo, M.D.
George I. Papkostas, M.D.
Jagoda Pasic, M.D., Ph.D.
Michael Posternak, M.D.
Lawrence H. Price, M.D.
Mark Hyman Rapaport, M.D.
Steven P. Roose, M.D.
Anthony J. Rothschild, M.D.
Peter Roy-Byrne, M.D.
John P.D. Shemo, M.D., D.F.A.P.A.
103
David A. Solomon, M.D.
Robert Stern, M.D., Ph.D.
Joel E. Streim, M.D.
Shona Sturgeon, M.Soc.Sc.
Richard P. Swinson, M.D., F.R.C.P.C., F.R.C.Psych.
Michael J. Telch, Ph.D.
John Chapman Urbaitis, M.D.
Eduard Vieta, M.D., Ph.D.
Karen Dineen Wagner, M.D., Ph.D.
Risa B. Weisberg, Ph.D.
Myrna M. Weissman, Ph.D.
Kimberly A. Yonkers, M.D.
Mark Zimmerman, M.D.
American Academy of Neurology
American Academy of Psychoanalysis and Dynamic
Psychiatry
American Association for Marriage and Family Therapy
American Association of Emergency Psychiatry
American Geriatrics Society
American Group Psychotherapy Association
American Mental Health Counselors Association
American Neuropsychiatric Association
Association for Behavior and Cognitive Therapy
Association of Family Psychiatrists
Canadian Psychiatric Association
Community Mental Health Council, Inc.
National Association of Social Workers
Society for Adolescent Medicine
World Federation for Mental Health
ACKNOWLEDGMENT
Massimiliano Beghi, M.D., assisted with the evidence review for this guideline.
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The following coding system is used to indicate the nature of the supporting evidence in the references:
[A]
Randomized double-blind clinical trial. A study of an intervention in which subjects are prospectively followed over time, there are treatment and control groups, subjects are randomly assigned to the two
groups, both the subjects and the investigators are blind to the assignments.
[A−] Randomized clinical trial. Same as above but not double-blind.
[B]
Clinical trial. A prospective study in which an intervention is made and the results of that intervention are
tracked longitudinally; study does not meet standards for a randomized clinical trial.
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
10 4
APA PRACTICE GUIDELINES
[C]
Cohort or longitudinal study. A study in which subjects are prospectively followed over time without any specific intervention.
[D] Case-control study. A study in which a group of patients and a group of control subjects are identified in the
present and information about them is pursued retrospectively or backward in time.
[E]
Review with secondary data analysis. A structured analytic review of existing data, e.g., a meta-analysis or a
decision analysis.
[F]
Review. A qualitative review and discussion of previously published literature without a quantitative synthesis of the data.
[G] Other. Textbooks, expert opinion, case reports, and other reports not included above.
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